[go: up one dir, main page]

WO1993004040A1 - Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them - Google Patents

Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them Download PDF

Info

Publication number
WO1993004040A1
WO1993004040A1 PCT/GB1992/001503 GB9201503W WO9304040A1 WO 1993004040 A1 WO1993004040 A1 WO 1993004040A1 GB 9201503 W GB9201503 W GB 9201503W WO 9304040 A1 WO9304040 A1 WO 9304040A1
Authority
WO
WIPO (PCT)
Prior art keywords
phenyl
methyloxy
trifluoromethyl
phenylpiperidine
cis
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Ceased
Application number
PCT/GB1992/001503
Other languages
French (fr)
Inventor
Raymond Baker
Timothy Harrison
Christopher John Swain
Brian John Williams
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Organon Pharma UK Ltd
Original Assignee
Merck Sharp and Dohme Ltd
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Priority claimed from GB919117934A external-priority patent/GB9117934D0/en
Priority claimed from GB919125619A external-priority patent/GB9125619D0/en
Priority claimed from GB929204119A external-priority patent/GB9204119D0/en
Priority to US08/196,269 priority Critical patent/US5459270A/en
Priority to AT92917251T priority patent/ATE136885T1/en
Priority to AU24138/92A priority patent/AU661711B2/en
Priority to JP5504179A priority patent/JPH06510034A/en
Application filed by Merck Sharp and Dohme Ltd filed Critical Merck Sharp and Dohme Ltd
Priority to DE69210029T priority patent/DE69210029T2/en
Priority to EP92917251A priority patent/EP0600952B1/en
Publication of WO1993004040A1 publication Critical patent/WO1993004040A1/en
Anticipated expiration legal-status Critical
Ceased legal-status Critical Current

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D401/00Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom
    • C07D401/02Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings
    • C07D401/04Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings directly linked by a ring-member-to-ring-member bond
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/02Drugs for disorders of the nervous system for peripheral neuropathies
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P29/00Non-central analgesic, antipyretic or antiinflammatory agents, e.g. antirheumatic agents; Non-steroidal antiinflammatory drugs [NSAID]
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P43/00Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D205/00Heterocyclic compounds containing four-membered rings with one nitrogen atom as the only ring hetero atom
    • C07D205/02Heterocyclic compounds containing four-membered rings with one nitrogen atom as the only ring hetero atom not condensed with other rings
    • C07D205/04Heterocyclic compounds containing four-membered rings with one nitrogen atom as the only ring hetero atom not condensed with other rings having no double bonds between ring members or between ring members and non-ring members
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D207/00Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom
    • C07D207/02Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
    • C07D207/04Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members
    • C07D207/10Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
    • C07D207/12Oxygen or sulfur atoms
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D211/00Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings
    • C07D211/04Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
    • C07D211/06Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members
    • C07D211/36Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
    • C07D211/40Oxygen atoms
    • C07D211/42Oxygen atoms attached in position 3 or 5
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D211/00Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings
    • C07D211/04Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
    • C07D211/68Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having one double bond between ring members or between a ring member and a non-ring member
    • C07D211/72Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having one double bond between ring members or between a ring member and a non-ring member with hetero atoms or with carbon atoms having three bonds to hetero atoms, with at the most one bond to halogen, directly attached to ring carbon atoms
    • C07D211/74Oxygen atoms
    • C07D211/76Oxygen atoms attached in position 2 or 6
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D409/00Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms
    • C07D409/02Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms containing two hetero rings
    • C07D409/04Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms containing two hetero rings directly linked by a ring-member-to-ring-member bond

Definitions

  • This invention relates to a class of azacyclic compounds, which are useful as tachykinin antagonists. More particularly, the compounds of the invention
  • the tachykinins are a group of naturally-occurring peptides found widely distributed throughout mammalian tissues, both within the central nervous system and in the peripheral nervous and circulatory systems.
  • the structures of three known mammalian tachykinins are as follows:
  • substance P is believed inter alia to be involved in the neurotransmission of pain sensations [Otsuka et al, "Role of Substance P as a Sensory
  • substance P is believed to be involved in the inflammatory response in diseases such as rheumatoid arthritis and
  • osteoarthritis [O' Byrne et al in Arthritis and Rheumatism (1990) 33 1023-8].
  • Other disease areas where tachykinin antagonists are believed to be useful are allergic conditions [Hamelet et al Can. J. Pharmacol. Physiol.
  • Substance P may also play a role in demyelinating diseases such as multiple sclerosis and amyotrophic lateral sclerosis [J. Luber-Narod et. al., poster to be presented at C.I.N.P. XVIIIth Congress, 28th June-2nd July, 1992, in press], and in disorders of bladder function such as bladder detrusor hyper-reflexia (Lancet,
  • tachykinins have utility in the following disorders: depression, dysthymic disorders , chronic obstructive airways disease, hypersensitivity disorders such as poison ivy,
  • vasospastic diseases such as angina and Reynauld's disease, fibrosing and collagen diseases
  • fibrosing and collagen diseases such as
  • scleroderma and eosinophillic fascioliasis reflex sympathetic dystrophy such as shoulder/hand syndrome
  • addiction disorders such as alcoholism, stress related somatic disorders, neuropathy, neuralgia, disorders related to immune enhancement or suppression such as systemic lupus erythmatosis
  • opthalmic disease such as conjuctivitis , vernal conjunctivitis , and the like
  • cutaneous diseases such as contact dermatitis, atropic dermatitis, urticaria, and other eczematoid dermatitis (European patent application no. 0 394 989).
  • peptide derivatives are likely to be of limited utility as therapeutic agents. It is for this reason that nonpeptide tachykinin antagonists are sought.
  • European patent application no. 0 436 334 discloses 4- to 7-membered azacyclic compounds substituted at the 3-position by a substituted amino moiety. The compounds are said to be tachykinin antagonists.
  • the present invention provides a compound of formula (I), or a salt or prodrug thereof:
  • wnerein n is 1, 2 or 3 and where any carbon atom of (CH 2 ) n may be substituted by R 4 and/or R 5 ;
  • X represents O or S
  • R 1 represents phenyl optionally substituted by 1, 2 or 3 groups selected from C 1-6 alkyl, C 2-6 alkenyl,
  • R 2 represents aryl selected from phenyl
  • heteroaryl selected from indazolyl, thienyl, furyl, pyridyl, thiazolyl, tetrazolyl and quinolyl;
  • each aryl or heteroaryl moiety may be substituted by C 1-6 alkyl, C 1-6 alkoxy, halo or trifluoromethyl;
  • R 4 and ⁇ 5 each independently represent H, halo, CH 2 OR 9 , C 1-6 alkyl, oxo, CO 2 R 10 or CONR 10 R 11 ;
  • R 8 represents H, COR 9 , CO 2 R 10 , COCONR 10 R 11 , COCO 2 R 10 or C 1-6 alkyl optionally substituted by a group selected from (CO 2 R 10 , CONR 10 R 11 , hydroxy, cyano, COR 9 , NR 10 R 11 , C(NOH)NR 10 R 11 , CONHphenyl (C 1-4 alkyl), COCO 2 R 10 ,
  • R a and R b each independently represent H, C 1-6 alkyl, phenyl or trifluoromethyl
  • R 9 represents H, C 1-6 alkyl or phenyl
  • R 10 and R 11 each independently represent H or
  • n is 2 or 3; R 4 and R 5 each independently represent H, halo, C 1-6 alkyl, CO 2 R 10 or CONR 10 R 11 ; and R 8 represents H, COR 9 or
  • C 1-6 alkyl optionally substituted by a group selected from (CO 2 R 10 , CONR 10 R 11 and phenyl optionally substituted by C 1-6 alkyl, C 1-6 alkoxy, halo or trifluoromethyl).
  • a further subgroup of compounds according to the invention is represented by compounds wherein n is 2 or 3;
  • R 2 represents phenyl or benzhydryl wherein any of the phenyl rings of the phenyl or benzhydryl moieties may optionally be substituted by halo or trifluoromethyl;
  • R 4 and R 5 each independently represent H, C 1-6 alkyl or
  • R 8 represents H or C 1-6 alkyl.
  • n is 2 or 3, more preferably 3.
  • X represents O.
  • R 1 represents substituted phenyl.
  • suitable substituents include C 1-6 alkyl especially C 1-4 alkyl such as methyl and tbutyl, nitro, trifluoromethyl, trimethylsilyl, halo such as bromo, chloro and iodo, carboxy, cyano, C 1-6 alkoxy such as methoxy and amino.
  • R 1 represents phenyl substituted by one or more groups selected from methyl, trifluoromethyl and halo, especially chloro.
  • R 1 represents disubstituted phenyl.
  • Suitable values for the group R 2 include aryl such as substituted or unsubstituted phenyl, 5-membered heteroaryl such as thienyl, 6-membered heteroaryl such as pyridyl, and benzhydryl.
  • R 2 represents unsubstituted
  • substituents include C 1-6 alkyl, such as methyl, and halo, such as chloro. Particularly preferred are compounds of formula (I) wherein R 2 represents unsubstituted phenyl.
  • Suitable values for R 4 and R 5 include H, C 1-6 alkyl, especially methyl, CH 2 OR 9 such as hydroxymethyl and oxo.
  • the substituents R 4 and R 5 may be located on any combination
  • R 4 and R 5 represents H.
  • R 4 and R 5 both represent H.
  • one of R 4 and R 5 is H and the other is 6- hydroxymethyl .
  • R 8 examples include H, COR 9 , such as CHO and COCH 3 , CO 2 R 10 , such as CO 2 C 1-6 alkyl e.g. CO 2 C 1-4 alkyl such as CO 2 t-butyl, COCONR 10 R 11 , such as COCONH 2 ,
  • COCO 2 R 10 such as COCO 2 C 1-4 alkyl, for example, COCO 2 CH 3 , C 1-6 alkyl, such as methyl, and substituted C 1-6 alkyl e.g. substituted C 1-3 alkyl such as methyl, ethyl or n-propyl, such as C 1-6 alkyl substituted by CO 2 R 10 , especially
  • CONHphenyl (C 1-4 alkyl), especially CONHbenzyl
  • C 1-6 alkoxy such as methoxy or trifluoromethyl.
  • R 8 represents H.
  • R 8 represents C 1-6 alkyl substituted by CO 2 R 10 or CONR 10 R 11 , more preferably R 8 represents CH 2 CO 2 R 10 , CH(CH 3 )CO 2 R 10 , CH 2 CONR 10 R 11 or CH (CH 3 ) CONR 10 R 11 ,
  • alkyl, alkenyl and alkynyl groups referred to with respect to the formulae herein may represent
  • suitable alkyl groups include methyl, ethyl, n- or iso-propyl, n-, sec-, isoor tert-butyl, cyclopropyl, cyclobutyl, cyclopentyl or cyclohexyl, and cycloalkyl-alkyl groups such as
  • suitable alkenyl groups include vinyl and allyl
  • suitable alkynyl groups include propargyl
  • halo as used herein includes fluoro, chloro, bromo and iodo.
  • the salts of the compounds of formula (I) will be non-toxic pharmaceutically acceptable salts.
  • Other salts may, however, be useful in the preparation of the compounds according to the invention (such as the dibenzoyltartrate salts) or of their nontoxic pharmaceutically acceptable salts.
  • Suitable pharmaceutically acceptable salts of the compounds of this invention include acid addition salts which may, for example, be formed by mixing a solution of the compound according to the invention with a solution of a
  • salts of amine groups may also comprise quaternary ammonium salts in which the amino nitrogen atom carries a suitable organic group such as an alkyl, alkenyl, alkynyl or aralkyl moiety.
  • suitable pharmaceutically acceptable salts thereof may include metal salts such as alkali metal salts, e.g. sodium or potassium salts; and alkaline earth metal salts, e.g. calcium or magnesium salts.
  • Preferred salts of the compounds according to the invention include the hydrochloride, hydrobromide and ptoluenesulphonic acid salts, especially the hydrobromide salt.
  • the present invention includes within its scope prodrugs of the compounds of formula (I) above.
  • prodrugs will be functional derivatives of the compounds of formula I which are readily convertible in vivo into the required compound of formula (I).
  • the compounds according to the invention may exist both as enantiomers and as diastereomers. It is to be understood that all such isomers and mixtures thereof are encompassed within the scope of the present invention.
  • a particular sub-class of compounds according to the invention is represented by compounds of formula (Ia), and salts and prodrugs thereof:
  • R 2 , R 8 and X are as defined for formula (I);
  • R 20 and R 21 independently represent H, C 1-6 alkyl, C 1-6 alkenyl, C 1-6 alkynyl, halo, cyano, nitro,
  • R b are as previously defined;
  • R 22 represents H, C 1-6 alkyl, CH 2 OR 9 or oxo,
  • R 20 and R 21 include H, methyl, butyl, halo, trimethylsilyl, trifluoromethyl, nitro, carboxy, cyano and amino.
  • R 20 and R 21 are both other than H and are located at the 3- and 5- positions of the phenyl ring. More preferably R and
  • R 21 each represent trifluoromethyl.
  • R 22 may be located on any available carbon atom of the piperidine ring.
  • R 22 when R 22 is C 1-6 alkyl or CH 2 OR 9 , it may be located at the 2-, 3-, or 6-position of the piperidine ring, preferably the 6-position.
  • R 22 is oxo, it is preferably located at the 6-position.
  • the invention also provides pharmaceutical
  • compositions comprising one or more compounds of this invention in association with a pharmaceutically
  • compositions are in unit dosage forms such as tablets, pills, capsules, powders, granules, sterile parenteral solutions or suspensions, or suppositories, for oral, parenteral or rectal administration.
  • a pharmaceutical carrier e.g. conventional
  • tableting ingredients such as corn starch, lactose, sucrose, sorbitol, talc, stearic acid, magnesium
  • a solid preformulation composition containing a homogeneous mixture of a compound of the present invention, or a nontoxic pharmaceutically acceptable salt thereof.
  • a solid preformulation composition containing a homogeneous mixture of a compound of the present invention, or a nontoxic pharmaceutically acceptable salt thereof.
  • the active ingredient is dispersed evenly throughout the composition so that the composition may be readily subdivided into equally effective unit dosage forms such as tablets, pills and capsules.
  • This solid preformulation composition is then subdivided into unit dosage forms of the type described above containing from 0.1 to about 500 mg of the active ingredient of the present invention.
  • the tablets or pills of the novel composition can be coated or otherwise compounded to provide a dosage form affording the
  • the tablet or pill can comprise an inner dosage and an outer dosage component, the latter being in the form of an envelope over the former.
  • the two components can be separated by an enteric layer which serves to resist disintegration in the stomach and permits the inner component to pass intact into the duodenum or to be delayed in release.
  • enteric layers or coatings such materials including a number of polymeric acids and mixtures of polymeric acids with such materials as shellac, cetyl alcohol and cellulose
  • aqueous solutions suitably flavoured syrups, aqueous or oil suspensions, and flavoured emulsions with edible oils such as cottonseed oil, sesame oil, coconut oil or peanut oil, as well as elixirs and similar pharmaceutical vehicles.
  • Suitable dispersing or suspending agents for aqueous suspensions include synthetic and natural gums such as tragacanth, acacia, alginate, dextran, sodium carboxymethylcellulose, methylcellulose, polyvinylpyrrolidone or gelatin.
  • the present invention futher provides a process for the preparation of a pharmaceutical composition
  • the compounds of formula (I) are of value in the treatment of a wide variety of clinical conditions which are characterised by the presence of an excess of
  • tachykinin in particular substance P, activity.
  • disorders of the central nervous system such as anxiety, depression, psychosis and schizophrenia;
  • neurodegenerative disorders such as dementia, including senile dementia of the Alzheimer type, Alzheimer's disease and Down's syndrome; demyelinating diseases such as MS and ALS and other neuropathological disorders such as peripheral neuropathy, for example, diabetic and chemotherapy-induced neuropathy, and postherpetic and other neuralgias; respiratory diseases such as chronic obstrucutive airways disease, bronchopneumonia,
  • bronchospasm and asthma inflammatory diseases such as inflammatory bowel disease, psoriasis, fibr ⁇ sitis, osteoarthritis and rheumatoid arthritis; allergies such as eczema and rhinitis; hypersensitivity disorders such as poison ivy; ophthalmic diseases such as
  • cutaneous diseases such as contact dermatitis, atropic dermatitis, urticaria, and other eczematoid dermatitis; addiction disorders such as alcoholism; stress related somatic disorders; reflex sympathetic dystrophy such as shoulder/hand syndrome; dysthymic disorders; adverse immunological reactions such as rejection of transplanted tissues and disorders related to immune enhancement or suppression such as systemic lupus erythematosis; gastrointestinal (GI) disorders and diseases of the GI tract such as disorders associated with the neuronal control of viscera such as ulcerative colitis, Crohn's disease and incontinence; disorders of bladder function such as bladder detrusor hyper-reflexia; fibrosing and collagen diseases such as scleroderma and eosinophilic fascioliasis ; disorders of blood flow caused by
  • vasodilation and vasospastic diseases such as angina, migraine and Reynaud's disease; and pain or nociception, for example, that attributable to or associated with any of the foregoing conditions, especially the transmission of pain in migraine.
  • the compounds of formula (I) may suitably be used in the treatment of disorders of the central nervous system such as anxiety, psychosis and schizophrenia; neurodegenerative disorders such as senile dementia of the Alzheimer type,
  • Alzheimer's disease and Down's syndrome a respiratory diseases such as bronchospasm and asthma; inflammatory diseases such as inflammatory bowel disease,
  • GI gastrointestinal
  • diseases of the GI tract such as disorders associated with the neuronal control of viscera such as ulcerative colitis, Crohn's disease and incontinence; disorders of blood flow caused by vasodilation; and pain or nociception, for example, that attributable to or associated with any of the foregoing conditions or the transmission of pain in migraine.
  • the compounds of formula (I) are particularly useful in the treatment of pain or nociception and/or
  • neuropathy such as diabetic or peripheral neuropathy and chemotherapy-induced neuropathy, postherpetic and other neuralgias, asthma,
  • osteroarthritis rheumatoid arthritis and especially migraine.
  • the present invention further provides a compound of formula (I) for use in therapy.
  • the present invention provides a compound of formula (I) for use in the manufacture of a medicament for the treatment of physiological disorders associated with an excess of tachykinins, especially substance P.
  • the present invention also provides a method for the the treatment or prevention of
  • a suitable dosage level is about 0.001 to 50 mg/kg per day, in particular about 0.01 to about 25 mg/kg, such as from about 0.05 to about 10 mg/kg per day.
  • a suitable dosage level is about 0.001 to 50 mg/kg per day, in particular about 0.01 to about 25 mg/kg, such as from about 0.05 to about 10 mg/kg per day.
  • a suitable dosage level is about 0.001 to 25 mg/kg per day, preferably about 0.005 to 10 mg/kg per day, and especially about 0.005 to 5 mg/kg per day.
  • the compounds may be administered on a regimen of 1 to 4 times per day, preferably once or twice per day.
  • the compounds according to the invention may be prepared by a process which comprises reacting a compound of formula (III) with a compound of formula (IV):
  • R 1 , R 2 , R 4 , R and n are as defined for formula (I)
  • R 8 is as defined for formula (I) except that, when R is H it is replaced by a suitable protecting group, such as CO 2 (C 1-6 alkyl); and one of R 30 and R 31 represents a ieaving group and the other of R 30 and R 31 represents XH, where X is as defined for formula (I); in the
  • R 30 represents XH and R 31 represents a leaving group.
  • Suitable leaving groups include halo, e.g. chloro, bromo or iodo, or sulphonate derivatives such as tosylate or mesylate.
  • reaction is conveniently carried out in a suitable organic solvent, such as an ether, e.g. 1,2- dimethoxyethane, at a temperature in the region of 0°C.
  • suitable organic solvent such as an ether, e.g. 1,2- dimethoxyethane
  • Favoured bases of use in the reaction include alkali metal amides and hydrides, such as potassium
  • potassium bis (trimethylsilyl) amide is used.
  • Compounds of formula (I) may also be prepared from different compounds of formula (I) by interconversion processes.
  • interconversion processes may be used to vary the group R 8 .
  • compounds of formula (I) wherein R 8 is other than H may be prepared from the corresponding compounds of formula (I) wherein R 8 is H by conventional methods, such as reaction with a compound R 8 -Hal, where Hal represents halo, in the presence of a base.
  • Suitable reagents and conditions will be readily apparent to those skilled in the art and are illustrated by the accompanying Examples.
  • Suitable bases include organic bases, such as tertiary amines, e.g. triethylamine, and inorganic bases, such as alkali metal carbonates, e.g.
  • R 2 , R 4 , R 5 and R 8 are as defined for formula III above, q is 1 or 2 and R 50 is an optional carbonyl group, by reduction.
  • Suitable reducing agents will be readily apparent to one skilled in the art and include, for example, metallic hydrides, such as lithium aluminium hydride or, preferably, sodium borohydride.
  • CO 2 (C 1-6 alkyl), may be prepared by reaction of compounds of formula (VI) with compounds of formula (VII):
  • Suitable bases include alkali metal hydrides, such as sodium hydride, and alkali metal alkoxides, such as sodium butoxide.
  • the reaction is conveniently effected in a suitable organic solvent, such as a hydrocarbon, for example, benzene or toluene, or an ether, for example tetrahydrofuran.
  • R 5 represents CO 2 (C 1-6 alkyl) (VB), may be prepared by reaction of a compound of formula (VI) with a compound of formula (VIIA)
  • Hal represents halo, such as chloro, bromo or iodo, and CO 2 R e is as above defined, in the presence of a base, as above described.
  • Compounds of formula (V) wherein one or both of R 4 and R 5 represents halo, C 1-6 alkyl, CONR 10R11 or CO 2 R 10 may be prepared from appropriately substituted analogues of the compounds of formulae (VI), (VII) and (VIIA), or by appropriate interconversion procedures which will be readily apparent to those skilled in the art.
  • C 1-6 alkyl may be prepared from the corresponding compounds of formula (VI) wherein R d is hydrogen (VIB), by conventional methods.
  • R 2 is as above defined and Hal is halo, such as bromo, chloro or iodo, in the presence of a base, followed by hydrolysis and suitable modification of the nitrogen substituent using conventional methods.
  • Suitable bases of use in the reaction include metal hydroxides, for example, sodium hydroxide.
  • the reaction is conveniently effected in a mixture of water and a suitable organic solvent, such as a hydrocarbon, for example, toluene, in the presence of a phase transfer catalyst, such as benzyltrimethylammonium chloride.
  • Hydrolysis is conveniently effected by heating a solution of the product of reaction between the compound of formula (IX) and R 2 -Hal in concentrated hydrochloric acid, at reflux.
  • novel compounds may be prepared in racemic form, or individual enantiomers may be prepared either by enantiospecific synthesis or by resolution.
  • intermediate alcohols of formula (III), wherein R 30 is OH may be resolved into their component enantiomers by standard techniques, such as the formation of
  • protecting groups may be removed at a convenient
  • Boc t-butoxycarbonyl
  • Trifluoro acetic acid ( 3ml ) wa s adde d to 1 -t- butyloxycarbonyl-3-((3,5-dimethylphenyl)methyloxy)-2- phenylpiperidine (800mg Example 2d) under nitrogen and the solution was stirred at 23°C for 1h. Excess trifluoroacetic acid was removed in vacuo, and the residue was partitioned between 2M sodium hydroxide and dichloromethane. The layers were separated, and the aqueous phase was extracted twice with dichloromethane. The combined organic phases were dried
  • Acetyl chloride (0.26ml, 3.66mmol) was added dropwise with stirring to anhydrous methanol (3.7ml) and the resultant solution was added to a solution of cis-3-((3,5- dimethylphenyl)methyloxy)-2-phenylpiperidine (360mg, 1.22mmol) in anhydrous methanol (1ml).
  • (+)-cis-3-((3,5-bis(trifluoromethyl) phenyl)methyloxy)-2-phenyl piperidine prepared from hydrochloride salt (Example 5, 1.0g) by partitioning between aqueous sodium carbonate and dichloromethane) in dry dichloromethane (5ml) was added pyridine (0.67ml), acetic anhydride (0.79ml) and 4,4-dimethylamine pyridine (10mg). After the solution had been stirred for 3h at 23°C, saturated sodium bicarbonate solution was added and the organic phase dried (MgSO 4 ), evaporated in vacuo and chromatographed on silica gel to give the title compound as an oil. Found: C,59.51;
  • the title compound was prepared from (+)-cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine (prepared from the hydrochloride salt, Example5 )(0.5g) and formic-acetic anhydride (prepared from 90% formic acid (1.0ml) and acetic anhydride (3ml) at 60°C for 30 minutes) in tetrahydrofuran for 48h at 23°C. The solvent was evaporated in ⁇ acuo and the residue partitioned between diochloromethane and saturated aqueous sodium bicarbonate solution, dried
  • reaction mixture was stirred at 23°C for 1h, then added to a cooled (- 10°C) solution of N-Boc phenyl glycine aldehyde (3.2g) in dry tetrahydrofuran (20ml), the mixture was allowed to warm to 23°C, stirred for 1h then quenched by the addition of saturated aqueous ammonium chloride solution.
  • the reaction mixture was cooled to 5°C and quenched with methanol, then concentrated in vacuo.
  • the residue was dissolved in ethanol (30ml) and potassium carbonate (3.10g) was added and the mixture was heated at reflux for 6 hrs.
  • the solvent was removed in vacuo and the residue was partitioned between ethyl acetate (50ml) and water (100ml).
  • the aqueous layer was extracted with ethyl acetate (3 x50ml).
  • the combined organic extracts were dried (MgSO 4 ) and concentrated in vacuo.
  • EXAMPLE 24 cis-3-(3,5-Bis(trifluoromethyl)phenyl)methyloxy)- 2-(4-methylphenyl)piperidine hydrochloride salt a) Methyl-4-nitrobutyrate and 4-methylbenzaldehyde were treated in an analogous manner to that described in Example 2a to give 2-(4-methylphenyl)-3-nitro-6-oxopiperidine.
  • (+)-cis-3-Hydroxy-2-phenylpiperidine (Example 5c) was treated analogously to that described in Example 2c and then alkylated as described in Example 2d using 3-methyl-5- ( trimethylsilyl)benzyl bromide to give the title compound as a colourless oil.
  • Example 2c 1g was dissolved in dry dimethylformamide ( 10ml).
  • Sodium hydride 163mg, 80% dispersion in oil
  • Benzyl bromide 923mg was added and the mixture was stirred for 3h.
  • Excess sodium hydride was destroyed (ammonium chloride), the mixture was diluted with water and extracted with ethyl acetate ( 2 x 30ml). The organic washings were washed with brine, dried (MgSO 4 ) and evaporated.
  • the crude residue was purified by chromatography on silica using petrol/ether (70:30) as eluant. The product was dissolved in ether and the solution cooled to 0°C. Anhydrous hydrogen chloride was bubbled through the solution for 30 min.
  • the ether was then evaporated and the crude product was dispersed between ethyl acetate and aqueous potassium carbonate.
  • the organic extract was dried (MgSO 4 ) and evaporated and the crude oil was purified by chromatography on silica using 7% methanol in dichloromethane as eluant.
  • the product was dissolved in ethereal oxalic acid and recrystallised from ethyl acetate-ether, m.p. 150-151°C.
  • EXAMPLE 39 cis-N-(1-Acetamidooxime)-3-(3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine
  • the compound of Example 4 (800mg), hydroxylamine hydrochloride (188mg) and potassium carbonate (500mg) were suspended in ethanol ( 10ml) and the contents were heated at reflux for 5h. The mixture was cooled and evaporated and the residue was partitioned between dichloromethane and brine.
  • Example 4 The compound of Example 4 (5g), potassium carbonate (1.7g) and bromoacetonitrile (0.87ml) were suspended in dimethylformamide (15mi) and the mixture was stirred under nitrogen at 60°C for 3h. The mixture was cooled, diluted with water (200ml) and extracted with ethyl acetate (2 x 50ml). The organic extracts were washed with brine, dried (MgSO 4 ) and evaporated, affording a brown oil. This was purified on silica gel using ethyl acetate in petrol (10%) as eluant. This afforded the product as a colourless oil.
  • hydrochloride salt was prepared by dissolution in ethereal hydrogen chloride and the salt was recrystallised from diethyl ether-hexane, m.p.133-134°C.
  • Example 4 The title compound was prepared from cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine (Example 4) and 3,5-bis-trifluoromethyl benzyl bromide in an analogous manner to that described in Example 17. Found: C, 63.91; H, 3.62; N, 2.08. Calcd. for C 29 H 23 F 12 NO.0.3H 2 O C, 53.74; H, 3.89; N, 2.16%.
  • (+)-cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-1- carboxymethyl-2-phenyl piperidine (1g, Example 41), 1- hydroxybenzotriazole hydrate (1.2g), 1-(3-dimethylaminopropyl)- 3-ethyl-carbodiimide hydrochloride (1.66g), triethylamine (1.2ml) and diethylamine (0.55ml) were added together and the reaction was left stirring overnight at room temperature. The solvent was removed in vacuo and the residual yellow oil dispersed between water and ethyl acetate.
  • EXAMPLE 49 cis-3-((3,5-Bis(trifluoromethyl) ⁇ henyl)methyloxy- 1-(N-benzylcarboxamido)methyl-2-phenyl piperidinium hydrochloride
  • EXAMPLE 50 cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy- 1-(N-methylcarboxamido.methyl-2-phenyl piperidine
  • the title compound was prepared from cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-(carbomethoxy)methyl- 2-phenyl piperidine (Example 6) and methylamine in an analogous manner to that described in Example 7.
  • the crude material was chromatographed on flash silica and eiuted with e thyl acetate : petrol ( 1 : 9 ) to affo rd me thyl - O -( 3 , 5 - dimethylbenzyl)glycolate as a solid.
  • Example 2c The title compound was prepared from 1-t- butyloxycarbonyl-3-hydroxy-2-phenyl piperidine (Example 2c) and 3-bromobenzyl bromide in an analogous manner to that described in Example 2d, e, m.p.215-220°C; m/z (CI + ) 346 (MH); Analysis: Found: C, 56.90; H, 5.56; N, 3.68. Calcd for
  • Example 2c The title compound was prepared from 1-t- butyloxycarbonyl-3-hydroxy-2-phenyl piperidine (Example 2c) and ⁇ -bromo-m-tolunitrile in an analogous manner to that described in Example 2d, e, m.p. 168-178°C; m/z (CI + ) 293 (MH).
  • Example 41 The compound of Example 41 was reacted with cyclopropylamine according to the procedure described in Example 43 to afford the title compound.
  • compositions according to the invention are provided.
  • the compound of formula (I), cellulose, lactose and a portion of the corn starch are mixed and granulated with
  • the resulting granulation is sieved, dried and blended with the remainder of the corn starch and the magnesium stearate. The resulting granulation is then compressed into tablets containing 1.0mg, 2.0mg, 25.0mg, 26.0mg, 50.0mg and 100mg of the active compound per tablet.
  • the sodium phosphate, citric acid monohydrate and sodium chloride are dissolved in a portion of the water.
  • the compound of formula (I) is dissolved or suspended in the solution and made up to volume.
  • the white soft paraffin is heated until molten.
  • the liquid paraffin and emulsifying wax are incorporated and stirred until dissolved.
  • the compound of formula (I) is added and stirring continued until dispersed. The mixture is then cooled until solid.
  • the cDNA for the human NK1R was cloned into the expression vector pCDM9 which was derived from pCDM8 (INVITROGEN) by inserting the
  • ampicillin resistance gene (nucleotide 1973 to 2964 from BLUESCRIPT SK+ (trademark, STRATAGENE, La Jolla, CA, USA)) into the Sac II site.
  • Transfection of 20 ug of the plasmid DNA into 10 million COS cells was achieved by electroporation in 800 ⁇ l of transfection buffer (135 mM NaCl, 1.2 mM CaCl 2 , 1.2 mM MgCl 2 , 2.4 mM K 2 HPO 4 , 0.6 mM
  • the cells were incubated in 10% fetal calf serum, 2 mM glutamine, 100U/ml penicillinstreptomycin, and 90% DMEM media (GIBCO, Grand Island, NY, USA) in 5% CO 2 at 37°C for three days before the binding assay.
  • the cDNA was subcloned into the vector pRcCMV (INVITROGEN).
  • Transfection of 20 ⁇ g of the plasmid DNA into CHO cells was achieved by electroporation in 800 ⁇ l of transfection buffer supplemented with 0.625 mg/ml Herring sperm DNA at 300 V and 950 ⁇ F using the IBI
  • GENEZAPPER (IBI). The transfected cells were incubated in CHO media [10% fetal calf serum, 100 U/ml penicillinstreptomycin, 2 mM glutamine, 1/500 hypoxanthinethymidine (ATCC), 90% IMDM media (JRH BIOSCIENCES,
  • KS Lenexa, KS, USA
  • G418 G418
  • COS or CHO cells is based on the use of 125 I-substance P ( 125 I-SP, from DU PONT, Boston, MA) as a radioactively labeled ligand which competes with unlabeled substance P or any other ligand for binding to the human NKIR.
  • 125 I-substance P 125 I-SP, from DU PONT, Boston, MA
  • Monolayer cell cultures of COS or CHO were dissociated by the non-enzymatic solution (SPECIALTY MEDIA, Lavellette, NJ) and resuspended in appropriate volume of the binding buffer (50 mM Tris pH 7.5, 5 mM MnCl 2 , 150 mM NaCl, 0.04 mg/ml bacitracin, 0.004 mg/ml leupeptin, 0.2 mg/ml BSA, 0.01 mM phosphoramidon) such that 200 ⁇ l of the cell suspension would give rise to about 10,000 cpm of specific 125 I-SP binding (approximately 50,000 to 200,000 cells).
  • the binding buffer 50 mM Tris pH 7.5, 5 mM MnCl 2 , 150 mM NaCl, 0.04 mg/ml bacitracin, 0.004 mg/ml leupeptin, 0.2 mg/ml BSA, 0.01 mM phosphoramidon
  • the binding assay 200 ⁇ l of cells were added to a tube containing 20 ⁇ l of 1.5 to 2.5 nM of 125 I-SP and 20 ⁇ l of unlabeled substance P or any other test compound. The tubes were incubated at 4°C or at room temperature for 1 hour with gentle shaking. The bound radioactivity was separated from unbound radioactivity by GF/C filter (BRANDEL, Gaithersburg, MD) which was prewetted with 0.1% polyethylenimine. The filter was washed with 3 ml of wash buffer (50 mM Tris pH 7.5, 5 mM MnCl 2 , 150 mM NaCl) three times and its radioactivity was determined by gamma counter.
  • wash buffer 50 mM Tris pH 7.5, 5 mM MnCl 2 , 150 mM NaCl
  • the activation of phospholiphase C by NKIR may also be measured in CHO cells expressing the human NKIR by determining the accumulation of inositol monophosphate which is a degradation product of IP 3 .
  • CHO cells are seeded in 12-well plate at 250,000 cells per well. After incubating in CHO media for 4 days, cells are loaded with 5 ⁇ Ci of 3 H-myoinositol in 1 ml of media per well by overnight incubation. The extracellular radioactivity is removed by washing with phosphate buffered saline. LiCl is added to the well at final concentration of 10 mM with or without the test compound, and incubation is continued at 37°C for 15 min.
  • Substance P is added to the well at final concentration of 0.3nM to activate the human NKIR. After 30 min of incubation at 37°C, the medium is removed and 0.1 N HCl is added. Each well is sonicated at 4°C and extracted with CHCl 3 /methanol (1:1). The aqueous phase is applied to a 1 ml Dowex AG 1X8 ion exchange column. The column is washed with 0.1 N formic acid followed by 0.025 M ammonium formate-0.1 N formic acid. The inositol monophosphate is eluted with 0.2 M ammonium formate-0.1 N formic acid and quantitated by beta counter.

Landscapes

  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Health & Medical Sciences (AREA)
  • General Chemical & Material Sciences (AREA)
  • Veterinary Medicine (AREA)
  • Public Health (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • General Health & Medical Sciences (AREA)
  • Medicinal Chemistry (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Animal Behavior & Ethology (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Engineering & Computer Science (AREA)
  • Neurology (AREA)
  • Neurosurgery (AREA)
  • Biomedical Technology (AREA)
  • Pain & Pain Management (AREA)
  • Rheumatology (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Nitrogen Condensed Heterocyclic Rings (AREA)
  • Nitrogen And Oxygen Or Sulfur-Condensed Heterocyclic Ring Systems (AREA)
  • Plural Heterocyclic Compounds (AREA)
  • Pyrrole Compounds (AREA)
  • Hydrogenated Pyridines (AREA)

Abstract

Compounds of formula (I), and salts and prodrugs thereof wherein n is 1, 2 or 3; X represents O or S; R?1 represents optionally substituted phenyl; R?2 represents aryl, heteroaryl, benzhydryl, or benzyl; R?4 and R?5 each independently represent H, halo, CH2?OR?9, C1-6?alkyl, oxo, CO2?R?10 or CONR?10R?11; R?8 represents H, COR?9, CO2?R?10 or optionally substituted C1-6?alkyl; R?9 represents H, C1-6?alkyl or phenyl; and R?10 and R?11 each independently represent H or C1-6?alkyl; are tachykinin antagonists. They and compositions thereof are useful in medicine.

Description

AZACYCLIC COMPOUNDS, PROCESSES FOR THEIR PREPARATION AND PHARMACEUTICAL COMPOSITIONS CONTAINING THEM This invention relates to a class of azacyclic compounds, which are useful as tachykinin antagonists. More particularly, the compounds of the invention
comprise an azacyclic ring system substituted by an arylmethyloxy or arylmethylthio moiety.
The tachykinins are a group of naturally-occurring peptides found widely distributed throughout mammalian tissues, both within the central nervous system and in the peripheral nervous and circulatory systems. The structures of three known mammalian tachykinins are as follows:
Substance P:
Arg-Pro-Lys-Pro-Gln-Gln-Phe-Phe-Gly-Leu-Met-NH2
Neurokinin A:
His-Lys-Thr-Asp-Ser-Phe-Val-Gly-Leu-Met-NH2
Neurokinin B:
Asp-Met-His-Asp-Phe-Phe-Val-Gly-Leu-Met-NH2
For example, substance P is believed inter alia to be involved in the neurotransmission of pain sensations [Otsuka et al, "Role of Substance P as a Sensory
Transmitter in Spinal Cord and Sympathetic Ganglia" in 1982 Substance P in the Nervous System, Ciba Foundation Symposium 91, 13-34 (published by Pitman) and Otsuka and Yanagisawa, "Does Substance P Act as a Pain Transmitter?" TIPS (Dec. 1987) 8 506-510], specifically in the
transmission of pain in migraine (B.E.B. Sandberg et al,
J. Med Chem, (1982) 25 1009) and in arthritis [Levine et al in Science (1984) 226 547-549]. These peptides have also been implicated in gastrointestinal (GI) disorders and diseases of the GI tract such as inflammatorv bowel disease [Mantyh et al in Neuroscience (1988) 25 (3) 817- 37 and D. Regoli in "Trends in Cluster Headache" Ed.
Sicuteri et al Elsevier Scientific Publishers, Amsterdam
(1987) page 85)]. It is also hypothesised that there is a neurogenic mechanism for arthritis in which substance P may play a role [Kidd et al "A Neurogenic Mechanism for Symmetrical Arthritis" in The Lancet, 11 November 1989 and Grόnblad et al "Neuropeptides in Synovium of Patients with Rheumatoid Arthritis and Osteoarthritis" in J.
Rheumatol. (1988) 15 (12) 1807-10]. Therefore, substance P is believed to be involved in the inflammatory response in diseases such as rheumatoid arthritis and
osteoarthritis [O' Byrne et al in Arthritis and Rheumatism (1990) 33 1023-8]. Other disease areas where tachykinin antagonists are believed to be useful are allergic conditions [Hamelet et al Can. J. Pharmacol. Physiol.
(1988) 66 1361-7], immunoregulation [Lotz et al Science (1988) 241 1218-21 and Kimball et al, J. Immunol. (1988) 141 (10) 3564-9] vasodilation, bronchospasm, reflex or neuronal control of the viscera [Mantyh et al, PNAS
(1988) 85 3235-9] and, possibly by arresting or slowing β-amyloid-mediated neurodegenerative changes [Yankner et al Science, (1990) 250, 279-82] in senile dementia of the Alzheimer type, Alzheimer's disease and Down's Syndrome.
Substance P may also play a role in demyelinating diseases such as multiple sclerosis and amyotrophic lateral sclerosis [J. Luber-Narod et. al., poster to be presented at C.I.N.P. XVIIIth Congress, 28th June-2nd July, 1992, in press], and in disorders of bladder function such as bladder detrusor hyper-reflexia (Lancet,
16th May, 1992, 1239).
It has furthermore been suggested that tachykinins have utility in the following disorders: depression, dysthymic disorders , chronic obstructive airways disease, hypersensitivity disorders such as poison ivy,
vasospastic diseases such as angina and Reynauld's disease, fibrosing and collagen diseases such as
scleroderma and eosinophillic fascioliasis, reflex sympathetic dystrophy such as shoulder/hand syndrome, addiction disorders such as alcoholism, stress related somatic disorders, neuropathy, neuralgia, disorders related to immune enhancement or suppression such as systemic lupus erythmatosis (European patent applicationno. 0 436 334), opthalmic disease such as conjuctivitis , vernal conjunctivitis , and the like , and cutaneous diseases such as contact dermatitis, atropic dermatitis, urticaria, and other eczematoid dermatitis (European patent application no. 0 394 989).
In view of their metabolic instability, peptide derivatives are likely to be of limited utility as therapeutic agents. It is for this reason that nonpeptide tachykinin antagonists are sought.
European patent application no. 0 436 334 discloses 4- to 7-membered azacyclic compounds substituted at the 3-position by a substituted amino moiety. The compounds are said to be tachykinin antagonists.
The present invention provides a compound of formula (I), or a salt or prodrug thereof:
Figure imgf000005_0001
wnerein n is 1, 2 or 3 and where any carbon atom of (CH2)n may be substituted by R4 and/or R5;
X represents O or S;
R1 represents phenyl optionally substituted by 1, 2 or 3 groups selected from C1-6alkyl, C2-6 alkenyl,
C2-6alkynyl, halo, cyano, nitro, trifluoromethyl,
trimethylsilyl, -ORa, SRa, SORa, SO2Ra, -NRaRb, -NRaCORb, -NRaCO2Rb, -CO2Ra or -CONRaRb;
R2 represents aryl selected from phenyl and
naphthyl; heteroaryl selected from indazolyl, thienyl, furyl, pyridyl, thiazolyl, tetrazolyl and quinolyl;
benzhydryl; or benzyl; wherein each aryl or heteroaryl moiety may be substituted by C1-6alkyl, C1-6alkoxy, halo or trifluoromethyl;
R 4 and Ε5 each independently represent H, halo, CH2OR9, C1-6alkyl, oxo, CO2R10 or CONR10R11 ;
R8 represents H, COR9, CO2R10, COCONR10R11, COCO2R10 or C1-6alkyl optionally substituted by a group selected from (CO2R10, CONR10R11, hydroxy, cyano, COR9, NR10R11, C(NOH)NR10R11 , CONHphenyl (C1-4alkyl), COCO2R10,
COCONR10 R11 and phenyl optionally substituted by one or more substituents selected from C1-6alkyl,C1-6 alkoxy, halo and trifluoromethyl);
Ra and Rb each independently represent H, C1-6alkyl, phenyl or trifluoromethyl;
R9 represents H, C1-6alkyl or phenyl; and
R10 and R11 each independently represent H or
C1-6alkyl.
One subgroup of compounds according to the invention is represented by compounds wherein n is 2 or 3; R4 and R5 each independently represent H, halo, C1-6alkyl, CO2R10 or CONR10R11; and R8 represents H, COR9 or
C1-6alkyl optionally substituted by a group selected from (CO2R10, CONR10R11 and phenyl optionally substituted by C1-6alkyl, C1-6alkoxy, halo or trifluoromethyl).
A further subgroup of compounds according to the invention is represented by compounds wherein n is 2 or 3; R2 represents phenyl or benzhydryl wherein any of the phenyl rings of the phenyl or benzhydryl moieties may optionally be substituted by halo or trifluoromethyl; R4 and R5 each independently represent H, C1-6alkyl or
CO2 (C1-6alkyl); and R8 represents H or C1-6alkyl.
Preferably n is 2 or 3, more preferably 3.
Preferably X represents O.
Preferably R1 represents substituted phenyl. When R1 is substituted phenyl suitable substituents include C1-6alkyl especially C1-4alkyl such as methyl and tbutyl, nitro, trifluoromethyl, trimethylsilyl, halo such as bromo, chloro and iodo, carboxy, cyano, C1-6alkoxy such as methoxy and amino. Preferably R1 represents phenyl substituted by one or more groups selected from methyl, trifluoromethyl and halo, especially chloro.
When monosubstituted, the substituent is suitably in the 3-position of the phenyl ring. More preferably R1 represents disubstituted phenyl. Particularly preferred are compounds of formula (I) wherein R1 represents 3,5- disubstituted phenyl, especially 3,5- bis (trifluoromethyl) phenyl.
Suitable values for the group R2 include aryl such as substituted or unsubstituted phenyl, 5-membered heteroaryl such as thienyl, 6-membered heteroaryl such as pyridyl, and benzhydryl.
Preferably R2 represents unsubstituted or
substituted phenyl or thienyl, pyridyl or benzhydryl.
When R is substituted phenyl, suitable phenyl
substituents include C1-6alkyl, such as methyl, and halo, such as chloro. Particularly preferred are compounds of formula (I) wherein R2 represents unsubstituted phenyl.
Suitable values for R4 and R5 include H, C1-6alkyl, especially methyl, CH2OR9 such as hydroxymethyl and oxo. The substituents R4 and R5 may be located on any
available ring carbon atom, including (except when they represent oxo) C-2 and C-3, but will preferably be located at the 6-position. Preferably at least one of R4 and R5 represents H. In one preferred group of compounds R4 and R5 both represent H. In a further preferred group of compounds one of R4 and R5 is H and the other is 6- hydroxymethyl .
Suitable values for R8 include H, COR9, such as CHO and COCH3, CO2R10, such as CO2C1-6alkyl e.g. CO2C1-4alkyl such as CO2t-butyl, COCONR10R11, such as COCONH2,
COCO2R10, such as COCO2C1-4alkyl, for example, COCO2CH3, C1-6alkyl, such as methyl, and substituted C1-6alkyl e.g. substituted C1-3alkyl such as methyl, ethyl or n-propyl,, such as C1-6alkyl substituted by CO2R10, especially
CO2CH3 and CO2H, CONR10R11 , especially CONH2, CONHCH3,
CONH(t-butyl), CONH(cyclopropyl) and CON (CH2CH3)2, cyano, C(NOH)NR10R11 , especially C(NOH)NH2,
CONHphenyl (C1-4 alkyl), especially CONHbenzyl, and
optionally substituted phenyl, especially unsubstituted phenyl and phenyl substituted by one or more of
C1-6alkoxy, such as methoxy or trifluoromethyl.
In one preferred group of compounds of formula (I), R8 represents H.
In a further preferred group of compounds of formula (I), R8 represents C1-6alkyl substituted by CO2R10 or CONR10R11, more preferably R8 represents CH2CO2R10, CH(CH3)CO2R10, CH2CONR10R11 or CH (CH3) CONR10R11 ,
especially CH2CO2CH3, CH (CH3) CO2CH3, CH2CONH2 or
CH(CH3)CONH2. The alkyl, alkenyl and alkynyl groups referred to with respect to the formulae herein may represent
straight, branched or cyclic groups or combinations thereof. Thus, for example, suitable alkyl groups include methyl, ethyl, n- or iso-propyl, n-, sec-, isoor tert-butyl, cyclopropyl, cyclobutyl, cyclopentyl or cyclohexyl, and cycloalkyl-alkyl groups such as
cyclopropylmethyl; suitable alkenyl groups include vinyl and allyl; and suitable alkynyl groups include propargyl.
The term "halo" as used herein includes fluoro, chloro, bromo and iodo.
For use in medicine, the salts of the compounds of formula (I) will be non-toxic pharmaceutically acceptable salts. Other salts may, however, be useful in the preparation of the compounds according to the invention (such as the dibenzoyltartrate salts) or of their nontoxic pharmaceutically acceptable salts. Suitable pharmaceutically acceptable salts of the compounds of this invention include acid addition salts which may, for example, be formed by mixing a solution of the compound according to the invention with a solution of a
pharmaceutically acceptable non-toxic acid such as hydrochloric acid, oxalic acid, fumaric acid, maleic acid, succinic acid, acetic acid, citric acid, tartaric acid, carbonic acid, phosphoric acid or ptoluenesulphonic acid. Salts of amine groups may also comprise quaternary ammonium salts in which the amino nitrogen atom carries a suitable organic group such as an alkyl, alkenyl, alkynyl or aralkyl moiety. Furthermore, where the compounds of the invention carry an acidic moiety, suitable pharmaceutically acceptable salts thereof may include metal salts such as alkali metal salts, e.g. sodium or potassium salts; and alkaline earth metal salts, e.g. calcium or magnesium salts. Preferred salts of the compounds according to the invention include the hydrochloride, hydrobromide and ptoluenesulphonic acid salts, especially the hydrobromide salt.
The present invention includes within its scope prodrugs of the compounds of formula (I) above. In general, such prodrugs will be functional derivatives of the compounds of formula I which are readily convertible in vivo into the required compound of formula (I).
Conventional procedures for the selection and preparation of suitable prodrug derivatives are described, for example, in "Design of Prodrugs", ed. H. Bundgaard, Elsevier, 1985.
The compounds according to the invention may exist both as enantiomers and as diastereomers. It is to be understood that all such isomers and mixtures thereof are encompassed within the scope of the present invention.
A particular sub-class of compounds according to the invention is represented by compounds of formula (Ia), and salts and prodrugs thereof:
Figure imgf000010_0001
Figure imgf000010_0002
( )
wherein R2, R8 and X are as defined for formula (I);
R20 and R21 independently represent H, C1-6alkyl, C1-6alkenyl, C1-6alkynyl, halo, cyano, nitro,
trifluoromethyl, trimethylsilyl, ORa, SRa SORa, SO2Ra, NRaRb, NRaCORb, NRaCO2Rb, CO2Ra or CONRaRb, where Ra and
Rb are as previously defined; and
R22 represents H, C1-6alkyl, CH2OR9 or oxo,
preferably H.
Particular values of R20 and R21 include H, methyl, butyl, halo, trimethylsilyl, trifluoromethyl, nitro, carboxy, cyano and amino. Preferably R20 and R21 are both other than H and are located at the 3- and 5- positions of the phenyl ring. More preferably R and
R21 each represent trifluoromethyl.
R22 may be located on any available carbon atom of the piperidine ring. In particular when R22 is C1-6alkyl or CH2OR9, it may be located at the 2-, 3-, or 6-position of the piperidine ring, preferably the 6-position. When
R22 is oxo, it is preferably located at the 6-position.
The invention also provides pharmaceutical
compositions comprising one or more compounds of this invention in association with a pharmaceutically
acceptable carrier. Preferably these compositions are in unit dosage forms such as tablets, pills, capsules, powders, granules, sterile parenteral solutions or suspensions, or suppositories, for oral, parenteral or rectal administration. For preparing solid compositions such as tablets, the principal active ingredient is mixed with a pharmaceutical carrier, e.g. conventional
tableting ingredients such as corn starch, lactose, sucrose, sorbitol, talc, stearic acid, magnesium
stearate, dicalcium phosphate or gums, and other
pharmaceutical diluents, e.g. water, to form a solid preformulation composition containing a homogeneous mixture of a compound of the present invention, or a nontoxic pharmaceutically acceptable salt thereof. When referring to these preformulation compositions as homogeneous, it is meant that the active ingredient is dispersed evenly throughout the composition so that the composition may be readily subdivided into equally effective unit dosage forms such as tablets, pills and capsules. This solid preformulation composition is then subdivided into unit dosage forms of the type described above containing from 0.1 to about 500 mg of the active ingredient of the present invention. The tablets or pills of the novel composition can be coated or otherwise compounded to provide a dosage form affording the
advantage of prolonged action. For example, the tablet or pill can comprise an inner dosage and an outer dosage component, the latter being in the form of an envelope over the former. The two components can be separated by an enteric layer which serves to resist disintegration in the stomach and permits the inner component to pass intact into the duodenum or to be delayed in release. A variety of materials can be used for such enteric layers or coatings, such materials including a number of polymeric acids and mixtures of polymeric acids with such materials as shellac, cetyl alcohol and cellulose
acetate.
The liquid forms in which the novel compositions of the present invention may be incorporated for
administration orally or by injection include aqueous solutions, suitably flavoured syrups, aqueous or oil suspensions, and flavoured emulsions with edible oils such as cottonseed oil, sesame oil, coconut oil or peanut oil, as well as elixirs and similar pharmaceutical vehicles. Suitable dispersing or suspending agents for aqueous suspensions include synthetic and natural gums such as tragacanth, acacia, alginate, dextran, sodium carboxymethylcellulose, methylcellulose, polyvinylpyrrolidone or gelatin. The present invention futher provides a process for the preparation of a pharmaceutical composition
comprising a compound of formula (I), which process comprises bringing a compound of formula (I) into
association with a pharmaceutically acceptable carrier or excipient.
The compounds of formula (I) are of value in the treatment of a wide variety of clinical conditions which are characterised by the presence of an excess of
tachykinin, in particular substance P, activity. These may include disorders of the central nervous system such as anxiety, depression, psychosis and schizophrenia;
neurodegenerative disorders such as dementia, including senile dementia of the Alzheimer type, Alzheimer's disease and Down's syndrome; demyelinating diseases such as MS and ALS and other neuropathological disorders such as peripheral neuropathy, for example, diabetic and chemotherapy-induced neuropathy, and postherpetic and other neuralgias; respiratory diseases such as chronic obstrucutive airways disease, bronchopneumonia,
bronchospasm and asthma; inflammatory diseases such as inflammatory bowel disease, psoriasis, fibrσsitis, osteoarthritis and rheumatoid arthritis; allergies such as eczema and rhinitis; hypersensitivity disorders such as poison ivy; ophthalmic diseases such as
conjunctivitis, vernal conjunctivitis, and the like;
cutaneous diseases such as contact dermatitis, atropic dermatitis, urticaria, and other eczematoid dermatitis; addiction disorders such as alcoholism; stress related somatic disorders; reflex sympathetic dystrophy such as shoulder/hand syndrome; dysthymic disorders; adverse immunological reactions such as rejection of transplanted tissues and disorders related to immune enhancement or suppression such as systemic lupus erythematosis; gastrointestinal (GI) disorders and diseases of the GI tract such as disorders associated with the neuronal control of viscera such as ulcerative colitis, Crohn's disease and incontinence; disorders of bladder function such as bladder detrusor hyper-reflexia; fibrosing and collagen diseases such as scleroderma and eosinophilic fascioliasis ; disorders of blood flow caused by
vasodilation and vasospastic diseases such as angina, migraine and Reynaud's disease; and pain or nociception, for example, that attributable to or associated with any of the foregoing conditions, especially the transmission of pain in migraine. For example, the compounds of formula (I) may suitably be used in the treatment of disorders of the central nervous system such as anxiety, psychosis and schizophrenia; neurodegenerative disorders such as senile dementia of the Alzheimer type,
Alzheimer's disease and Down's syndrome; respiratory diseases such as bronchospasm and asthma; inflammatory diseases such as inflammatory bowel disease,
osteoarthritis and rheumatoid arthritis; adverse
immunological reactions such as rejection of transplanted tissues; gastrointestinal (GI) disorders and diseases of the GI tract such as disorders associated with the neuronal control of viscera such as ulcerative colitis, Crohn's disease and incontinence; disorders of blood flow caused by vasodilation; and pain or nociception, for example, that attributable to or associated with any of the foregoing conditions or the transmission of pain in migraine.
The compounds of formula (I) are particularly useful in the treatment of pain or nociception and/or
inflammation and disorders associated therewith such as, for example, neuropathy, such as diabetic or peripheral neuropathy and chemotherapy-induced neuropathy, postherpetic and other neuralgias, asthma,
osteroarthritis, rheumatoid arthritis and especially migraine.
The present invention further provides a compound of formula (I) for use in therapy. According to a further or alternative aspect, the present invention provides a compound of formula (I) for use in the manufacture of a medicament for the treatment of physiological disorders associated with an excess of tachykinins, especially substance P. The present invention also provides a method for the the treatment or prevention of
physiological disorders associated with an excess of tachykinins, especially substance P, which method
comprises administration to a patient in need thereof of a tachykinin reducing amount of a compound of formula (I) or a composition comprising a compound of formula (I).
In the treatment of the conditions associated with an excess of tachykinins, a suitable dosage level is about 0.001 to 50 mg/kg per day, in particular about 0.01 to about 25 mg/kg, such as from about 0.05 to about 10 mg/kg per day. For example, in the treatment of
conditions involving the neurotransmission of pain sensations, a suitable dosage level is about 0.001 to 25 mg/kg per day, preferably about 0.005 to 10 mg/kg per day, and especially about 0.005 to 5 mg/kg per day. The compounds may be administered on a regimen of 1 to 4 times per day, preferably once or twice per day.
The compounds according to the invention may be prepared by a process which comprises reacting a compound of formula (III) with a compound of formula (IV):
Figure imgf000016_0001
( 1 1 1 ) ( i v ) wherein R1, R2, R4, R and n are as defined for formula (I), R8 is as defined for formula (I) except that, when R is H it is replaced by a suitable protecting group, such as CO2 (C1-6alkyl); and one of R30 and R31 represents a ieaving group and the other of R30 and R31 represents XH, where X is as defined for formula (I); in the
presence of a base, followed by deprotection, if
required.
Suitably R30 represents XH and R31 represents a leaving group.
Suitable leaving groups include halo, e.g. chloro, bromo or iodo, or sulphonate derivatives such as tosylate or mesylate.
The reaction is conveniently carried out in a suitable organic solvent, such as an ether, e.g. 1,2- dimethoxyethane, at a temperature in the region of 0°C. Favoured bases of use in the reaction include alkali metal amides and hydrides, such as potassium
bis (trimethylsilyl) amide or potassium hydride. Suitably, potassium bis (trimethylsilyl) amide is used.
Compounds of formula (I) may also be prepared from different compounds of formula (I) by interconversion processes. In particular, interconversion processes may be used to vary the group R8. For example, compounds of formula (I) wherein R8 is other than H may be prepared from the corresponding compounds of formula (I) wherein R8 is H by conventional methods, such as reaction with a compound R8-Hal, where Hal represents halo, in the presence of a base. Suitable reagents and conditions will be readily apparent to those skilled in the art and are illustrated by the accompanying Examples. Suitable bases include organic bases, such as tertiary amines, e.g. triethylamine, and inorganic bases, such as alkali metal carbonates, e.g. sodium carbonate. Compounds of formula (I) wherein R8 is COR9 may also be prepared from compounds of formula (I) wherein R8 is H by, for example, reaction with an appropriate acid anhydride. Compounds of formula (I) wherein R8 is C1-6alkyl may be prepared from corresponding compounds of formula (I) wherein R8 is COR9 by reduction using, for example, borane or a
borohydride such as sodium cyanoborohydride. Suitable procedures are described in the accompanying examples. Compounds of formula (I) wherein R8 is C1-6 alkyl
substituted by CONR10R11 may be prepared from
corresponding compounds of formula (I) wherein R8 is C1-6alkyl substituted by CO2R10 by treatment with ammonia or an amine of formula NR10R11.
The intermediates of formula (III) above wherein R30 is SH may be prepared from the corresponding
intermediates of formula (III) wherein R30 represents OH by treating the latter compound with Lawesson's reagent or phosphorus pentasulphide in a suitable solvent, e.g. pyridine, at ambient or elevated temperatures, suitably at reflux temperature.
Intermediates of formula (III) above wherein R30 is OH may be prepared from corresponding compounds of formula (V):
Figure imgf000018_0001
(V)
wherein R2, R4, R5 and R8 are as defined for formula III above, q is 1 or 2 and R50 is an optional carbonyl group, by reduction. Suitable reducing agents will be readily apparent to one skilled in the art and include, for example, metallic hydrides, such as lithium aluminium hydride or, preferably, sodium borohydride.
Intermediates of formula (III) wherein R30 is a leaving group may be prepared from compounds of formula (III) wherein R30 is OH, for example, by reaction with a thionyl halide, a mesyl halide or a tosyl halide.
Where they are not commercially available, the intermediates of formula (IV) above may be prepared by the procedures described in the accompanying Examples or by alternative procedures which will be readily apparent to one skilled in the art.
Compounds of formula (V) wherein q is 1, the
carbonyl group R50 is absent, and R5 represents
CO2 (C1-6alkyl), may be prepared by reaction of compounds of formula (VI) with compounds of formula (VII):
Figure imgf000019_0001
( V I ) ( V I I ) wherein R2 is as above defined, Rd represents C1-6alkyl and CO2R is R5; in the presence of a base.
Suitable bases include alkali metal hydrides, such as sodium hydride, and alkali metal alkoxides, such as sodium butoxide. The reaction is conveniently effected in a suitable organic solvent, such as a hydrocarbon, for example, benzene or toluene, or an ether, for example tetrahydrofuran.
Compounds of formula (V) wherein R50 is absent and
R5 represents CO2 (C1-6alkyl) (VB), may be prepared by reaction of a compound of formula (VI) with a compound of formula (VIIA)
Figure imgf000019_0002
(VI IA)
wherein q is 1 or 2 and Hal represents halo, such as chloro, bromo or iodo, and CO2Re is as above defined, in the presence of a base, as above described.
Further procedures for the preparation of compounds of formula (V) using the Dieckmann reaction will be apparent to those skilled in the art and are described in the accompanying examples. Compounds of formula (V) wherein R5 is other than CO2 (C1-6alkyl) may be prepared from compounds of formula
(V) wherein R5 represents CO2 (C1-6alkyl) by
decarboxylation using, for example, oxalic acid.
Alternatively, compounds of formula (V) wherein q is 2 may be prepared from enamines of formula (VIII):
Figure imgf000020_0001
(VI II)
according to the method of Cervinka et al, Collect.
Czech. Chem. Commun., 1988, 53, 308-10.
Compounds of formula (V) wherein q is 2 and the carbonyl group R50 is present may be prepared from intermediates of formula (IX):
Figure imgf000020_0002
(ιx)
by ozonolysis, or by means of the Nef reaction. Suitable reagents and conditions are described in Organic
Reactions, 38, 655.
Compounds of formula (V) wherein one or both of R4 and R5 represents halo, C1-6alkyl, CONR10R11 or CO2R10 may be prepared from appropriately substituted analogues of the compounds of formulae (VI), (VII) and (VIIA), or by appropriate interconversion procedures which will be readily apparent to those skilled in the art.
Intermediates of formula (VI) wherein Rd is
C1-6alkyl (VIA) may be prepared from the corresponding compounds of formula (VI) wherein Rd is hydrogen (VIB), by conventional methods.
Intermediates of formula (VIB) may be prepared from the compound of formula (X):
Figure imgf000021_0001
( X )
by reaction with a compound R2-Hal, wherein R2 is as above defined and Hal is halo, such as bromo, chloro or iodo, in the presence of a base, followed by hydrolysis and suitable modification of the nitrogen substituent using conventional methods.
Suitable bases of use in the reaction include metal hydroxides, for example, sodium hydroxide. The reaction is conveniently effected in a mixture of water and a suitable organic solvent, such as a hydrocarbon, for example, toluene, in the presence of a phase transfer catalyst, such as benzyltrimethylammonium chloride.
Hydrolysis is conveniently effected by heating a solution of the product of reaction between the compound of formula (IX) and R2-Hal in concentrated hydrochloric acid, at reflux.
The compound of formula (X) is commercially
available. Intermediates of formula (IX) are prepared as described in European Patent Application No. 0 436 334.
Compounds of formula R2-Hal may be prepared
according to the procedure described by E. J. Corey, Tetrahedron Lett., 1972, 4339.
Intermediates of formula (III) wherein n is 1 or 2 are novel compounds and constitute a further aspect of the present invention.
Where the above-described process for the
preparation of the compounds according to the invention gives rise to mixtures of stereoisomers these isomers may, if desired, be separated, suitably by conventional techniques such as preparative chromatography.
The novel compounds may be prepared in racemic form, or individual enantiomers may be prepared either by enantiospecific synthesis or by resolution. For example, intermediate alcohols of formula (III), wherein R30 is OH, may be resolved into their component enantiomers by standard techniques, such as the formation of
diastereomeric esters or amides, followed by
chromatographic separation or separation by fractional crystallization and removal of the chiral auxiliary. The diastereomeric alcohols can then be used to prepare optically pure compounds of formula (I).
During any of the above synthetic sequences it may be necessary and/or desirable to protect sensitive or reactive groups on any of the molecules concerned. This may be achieved by means of conventional protecting groups, such as those described in Protective Groups in Organic Chemistry, ed. J.F.W. McOmie, Plenum Press, 1973; and T.W. Greene and P.G.M. Wutts, Protective Groups in Organic Synthesis, John Wiley & Sons, 1991. The
protecting groups may be removed at a convenient
subsequent stage using methods known from the art. The following Examples illustrate the preparation of compounds according to the invention. "Celite" and
"Hiflo" are trade marks. THF means tetrahydrofuran. Boc means t-butoxycarbonyl.
EXAMPLE 1: cis 2-(Diphenylmethyl)-3-(3,5-dimethylbenzyloxy)- 1-methylpyrrolidine
a) Through a solution of 2-amino-3,3-diphenylpropanoic acid hydrochloride (35.0g, 126mmol) in methanol (500ml) was bubbled hydrogen chloride for 3h. The solution was stirred at room temperature for 120h and the solvent removed in vacuo. Addition of diethyl ether gave methyl 2-amino-3, 3- diphenylpropanoate hydrochloride, m.p. = 213-215°C (dec). 1H NMR (360MHz, DMSO-d6) 5 8.70 (3H, vbs), 7.20-7.57 (10H, m), 4.94 (1H, d, J = 11Hz), 4.36 (1H, d, J = 11Hz), 3.39 (3H, s). m/z
(CI+) 256 (MH).
b) To a solution of methyl 2-amino-3,3-diphenylpropanoate hydrochloride (Example 1a, 28.0g, 96mmol), chloroform (250ml), and 1.0M sodium carbonate (250ml) was added ethyl chloroformate (9.20ml, 96mmol). After the solution had been stirred for 18h the organic phase was separated, washed with 10% citric acid, water, saturated brine and dried (MgSO4). After removal of the solvent in vacuo the residue was recrystallised from hot methanol to give methyl 2- ethoxycarbonylamino-3,3-diphenylpropanoate, m.p. = 107-
109°C. Η NMR (250MHz, CDCl3) 5 7.18-7.33 (10H, m), 5.12 (1H, br t, J = 8.5Hz), 4.95 (1H, br d, J = 8.5Hz), 4.40 (1H, d, J = 8.0Hz), 4.06 (2H, q, J = 7.0Hz), 3.50 (3H, s), 1.17 (3H, t, J = 7.0Hz). m/z (CI+) 328 (MH).
c) To a suspension of 80% sodium hydride (2.48g, 83mmol) in benzene (50ml) was slowly added a solution of methyl 2- ethoxycarbonylamino-3,3-diphenylpropanoate (Example 1b, 27.0g, 83mmol) in benzene (200ml) and the mixture then heated at reflux for 1h. Ethanol (1.0ml) followed by ethyl acrylate (8.95ml, 83mmol) were added and the reaction heated at reflux for 2h, the solvent was then distilled off and the residue allowed to cool to room temperature. A solution of the residue in water was added to a concentrated sulphuric acid/ice mixture and the product extracted into ethyl acetate. The organic phase was washed with saturated brine and dried (MgSO4). The residue was chromatographed on silica gel in dichloromethane/methanol
(97:3) to give 1,4-bis(ethoxycarbonyl)-2-(diphenylmethyl)- pyrrolidin-3-one, m/z (CI+) 396 (MH). A solution of this oil in 1.0M oxalic acid was heated at reflux for 8h, cooled and the product extracted into chloroform. After separation the chloroform was removed in vacuo and the residue chromatographed on silica gel using ethyl acetate/hexane (1:4) as eluant to give 2-(diphenylmethyl)-1-ethoxycarbonylpyrrolidin- 3-one. 1H NMR (250MHz, CDCI3) δ 7.14-7.52 (10H, m), 4.80 (1H, br s), 4.68 (1H, vbr s), 4.18 (2H, br q), 3.94 (1H, vbs), 3.06 (1H, m), 2.34 (1H, m), 1.76 (1H, m), 1.22 (3H, t, J = 7.0Hz). m/z (CI+)
324 (MH).
d ) T o a s o l u t i o n o f 2 - ( di p h e n yl m e t h yl ) - 1 - ethoxycarbonylpyrrolidin-3-one (Example 1c, 5.75g, 18mmol) in ethanol (50ml) was added sodium borohydride (1.00g, 26mmol) and the mixture was stirred under nitrogen for 60h at room temperature. The reaction mixture was partitioned between 10% citric acid/ethyl acetate, the organic phase wsshed with saturated brine and dried (MgSC4). The solvent was removed in vacuo and the residue chromatographed on silica gel using ethyl acetate/hexane (2:3) as eluant. Recrystallisation from ethyl acetate/hexane gave cis-2-(diphenylmethyl)-3-hydroxy-1- ethoxycarbonylpyrrolidine, m.p. = 104-105°C. 1H NMR
(360MHz, CDCI3)δ 7.00-7.50 (10H, m), 4.78 (1H, dd, J = 9Hz and J = 7Hz), 4.46 (1H, dd, J = 8.0Hz and J = 7.0Hz), 4.32 (1H, d, J = 9Hz), 3.83 (2H, m), 3.47 (2H, m), 3.31 (1H, m), 2.10 (1H, m), 1.95 (1H, m), 1.00 (3H, t, J = 7.0Hz).
e) To a solution of cis-2-(diphenylmethyl)-3-hydroxy-1- ethoxycarbonylpyrrolidine (Example 1d, 1.00g, 3.1mmol) in ethylene glycol dimethyl ether (10.0ml) was added 0.5M potassium bis(trimethylsilyl)amide (9.00ml, 4.5mmol) and stirred at room temperature for ½h before addition of 3,5- dimethylbenzyl bromide (0.92g, 4.5mmol) in ethylene glycol dimethyl ether (2ml). After stirring for 18h the solvent was removed in vacuo and the residue partitioned between water/dichlorome thane. The organic phase was washed with saturated brine and dried (MgSO4). The residue, after removal of solvent in vacuo, was chromatographed on silica gel using ethyl acetate/hexane (2:3) as eluant to give cis-2- (diphenylmethyl)-3-(3,5-dimethylbenzyloxy)-1- ethoxycarbonylpyrrolidine. 1H NMR (360MHz, DMSO-d6)δ 7.05-7.46 (10H, m), 6.81 (1H, s), 6.58 (2H, s), 4.86 (1H, t, J = 7.0Hz), 4.42 (1H, d, 7.5Hz), 4.18 (1H, d, J = 12.0Hz), 4.11 (1H, m), 3.97 (1H, d, J = 12.0Hz), 3.83 (1H, m), 3.68 (1H, m), 3.31 (1H, m), 2.98 (1H, m), 2.19 (6H, s), 2.15 (1H, m), 1.95 (1H, m), 1.03 (3H, t, J = 7.0Hz). m/z (CI+) 444 (MH).
f) To a solution of cis-2-(diphenylmethyl)-3-(3,5- dimethylbenzyloxy)-1-ethoxycarbonylpyrrolidine (Example 1e, 0.500g, 1.1mmol) in tetrahydrofuran (5.0ml) was added 1.0M lithium aluminium hydride (5.0ml, 5 .0mmol) and then the solution heated at reflux for 1h. To the cooled solution was carefully added water (2ml), 4M sodium hydroxide (2ml) and water (4ml) followed by ethyl acetate. The suspension was filtered through Celite and the filtrate was washed with saturated brine and dried (MgSO4). Removal of the solvent in vacuo gave cis-2-(diphenylmethyl)-3-(3,5-dimethylbenzyloxy)-1- methylpyrrolidine. as an oil. 1H NMR (360MHz, CDCI3) δ 7.05- 7.43 (10H, m), 6.85 (1H, s), 6.68 (2H, s), 4.30 (1H, d, J = 15.0Hz), 4.01 (1H, d, J = 16.0Hz), 3.77 (1H, m), 3.63 (1H, d, J = 16.0Hz),
3.24 (2H, m), 2.30 (1H, m), 2.26 (6H, s), 1.91 (5H, m).
EXAMPLE 2: cis-3-((3,5-Dimethylphenyl)methyloxy)-2- phenylpiperidine hydrochloride salt
a) A solution of methyl-4-nitrobutyrate (23g, 0.156mol) and benzaldehyde (16ml, 0.156mol) in acetic acid (39ml) containing ammonium acetate (12.12g, 0.156mol) was heated at reflux under nitrogen for 2h. The reaction mixture was cooled to 5°C, whereby a pale-yellow solid crystallised. This was isolated by filtration, then dissolved in dichloromethane, washed cautiously with saturated aqueous sodium bicarbonate solution (2 x), then dried (MgSO4 ) and concentrated to leave a yellow solid. Recrystallisation from ethyl acetate provided 5-nitro-2-oxo-6- phenylpiperidine as a crystalline, white solid. 1H NMR (CDCI3) 5 7.46-7.26 (m), 6.0 (br s), 5.24 (dd, J = 1.4, 7.0Hz), 4.70 (m), 2.70-2.50 (m), 2.38-2.24 (m).
b) Potassium t-butoxide (1.68g, 15mmol) was added to a solution of 5-nitro-2-oxo-6-phenylpiperidine (3g, 13.6mmol; Example 2a) in a mixture of dichloromethane (50ml) and methanol (50ml) and the mixture was cooled to -78°C under nitrogen. Ozone was bubbled through the solution for 3h. A yellow-green solution resulted, and TLC indicated no starting material remained. The reaction mixture was purged with oxygen for 5 min to remove excess ozone, then dimethylsulfide
(7ml) was added and the reaction mixture was allowed to warm to 23°C. The solvent was removed in-vacuo, and the residue was partitioned between dichloromethane and water. The layers were separated, and the aqueous phase was extracted twice with dichloromethane. The combined organic extracts were washed with brine, then dried (K2CO3) and concentrated to leave 3,6- diketo-2-phenylpiperidine as a white solid.
This crude material was slurried in dry THF and added to lithium aluminium hydride (1M in THF, 50ml) then heated at reflux for 12h. After cooling to 23°C, the reaction mixture was quenched by the cautious addition of water (dropwise) under nitrogen, then 2M sodium hydroxide. The mixture was filtered through a pad of Hiflo, the filtrate was washed with brine, then dried (K2CO3) and concentrated to leave a yellow solid. Purification by silica-gel chromatography (CH2 Cl2 /MeOH/NH3 97:3 : 1 then CH2Cl2/MeOH 95:5) provided 3-hydroxy-2- phenylpiperidine as a mixture of cis- and trans- isomers. 1H
NMR (CDCI3) 7.44-7.20 (m), 3.84 (s), 3.76 (s), 3.54 (m), 3.4 (s), 3.3 (d, J = 8Hz), 3.26 (m), 3.04 (m), 2.78 (ddd, J = 2.9, 11.9, 11.9Hz), 2.70 (ddd, J = 2.9, 11.9, 11.9Hz), 2.18-1.78 (m), 1.48 (m). MS (El) m/z 177 (M).
c) Di-t-butyldicarbonate (1.36g, 6.2mmol) was added to a solution of 3-hydroxy-2-phenylpiperidine (1g, 5.6mmol, Example 2b) in dichloromethane (8ml) under nitrogen and the mixture stirred at 23°C for 3h. The solvent was removed in- vacuo, and the residue purified by silica- gel chromatography (CH2Cl2/MeOH/NH3 97:3:0.5) to provide cis- and trans-1-t- butyloxycarbonyl-3-hydroxy-2-phenylpiperidine as a clear, viscous oil. 1H NMR (CDCI3)δ 7.50-7.42 (m), 7.40-7.14 (m), 5.36 (d, J = 5.6Hz), 4.50 (m), 4.44 (m), 4.12-3.92 (m), 3.02 (ddd, J = 2.8, 12.6, 12.6Hz), 2.87 (ddd, J = 2.8, 12.6, 12.6Hz), 1.88-1.66 (m), 1.46 (s), 1.36 (s).
d) To a cooled (0°C) solution of 1-t-butyloxycarbonyl-3- hydroxy-2-phenylpiperidine (1.4g, 5.0mmol, Example 2c) in dry N,N-dimethylformamide (5ml) was added sodium hydride (80% dispersion in mineral oil; 182mg, 6.1mmol). The cooling bath was removed, and the reaction mixture stirred at 23°C for 0.5h.
A solution of 3,5-dimethylbenzylbromide (1.21g, 6.1mmol) in dry N,N-dimethylformamide ( 1ml) was added, and stirring continued at 23°C for 17h. The mixture was diluted with water (100ml) and extracted with dichloromethane (3 x 40ml). The combined organic extracts were washed with brine (1 x 30ml) then dried (K2CO3) and concentrated to leave a pale-yellow oil. Purification by silica gel chromatography (hexanes-ethyl acetate 19: 1→9:1→4: 1) provided a mixture of cis- and trans-1-t- butyloxycarbonyl-3-((3,5-dimethylphenyl)methyloxy)-2- phenylpiperidine as a clear, viscous oil. 1H NMR (CDCI3)δ 7.60 (d, J = 8.1Hz), 7.38-7.14 (m), 7.01 (s), 6.91 (s), 5.71 (br s), 5.60 (br s), 4.67 (app. d, J = 11.8Hz), 4.62 (d, J = 11.5Hz), 4.53 (d, J = 11.5Hz), 4.12 (m), 3.94 (br d, J = 13Hz), 3.82 (m), 2.84 (ddd, J =
3.3, 13.1, 13.1Hz), 2.67 (ddd, J = 3.3, 13.1, 13.1Hz), 2.39 (s), 2.31 (s), 1.99-1.82 (m), 1.69-1.49 (m), 1.51 (s), 1.47 (s).
e ) Trifluoro ace tic acid ( 3ml ) wa s adde d to 1 -t- butyloxycarbonyl-3-((3,5-dimethylphenyl)methyloxy)-2- phenylpiperidine (800mg Example 2d) under nitrogen and the solution was stirred at 23°C for 1h. Excess trifluoroacetic acid was removed in vacuo, and the residue was partitioned between 2M sodium hydroxide and dichloromethane. The layers were separated, and the aqueous phase was extracted twice with dichloromethane. The combined organic phases were dried
(K2CO3) and concentrated to leave a clear, colourless oil. Purification on silica gel (CH2Cl2/MeOH/NH3 97:3:0.5 then CH2Cl2/MeOH 95:5→90: 10→80:20) provided, in order of elution, trans-3 -( (3 , 5 -dimethylphenyl )methyloxy)-2- phenylpiperidine as a colourless oil. 1H NMR (CDCI3)δ 7.5-7.24
(m), 6.80 (s), 6.50 (s), 4.20 (d, J = 11Hz), 3.98 (d, J = 11Hz), 3.48 (d, J = 8.4Hz), 3.32 (ddd, J = 4.2, 9.8, 9.8Hz), 3.08 (m), 2.70 (ddd, J = 2.8, 12.6, 12.6Hz), 2.10 (m), 2.19 (s), 1.84-1.4 (m), and cis-3- ((3,5-dimethylphenyl)methyloxy)-2-phenylpiperidine as a colourless oil. 1H NMR (CDCI3) δ 7.4-7.2 (m), 6.55 (s), 6.31 (s), 4.33 (d, J = 12.2Hz), 4.10 (d, J = 12.2Hz), 3.78 (s), 3.63 (s), 3.26
(app. dt, J = 2.16, 2.16, 12.5Hz), 2.82 (ddd, J = 3.0, 3.0, 12.6Hz), 2.20 (s), 1.86 (m), 1.62 (m), 1.48 (m). m/z (CI+) 296 (MH).
Acetyl chloride (0.26ml, 3.66mmol) was added dropwise with stirring to anhydrous methanol (3.7ml) and the resultant solution was added to a solution of cis-3-((3,5- dimethylphenyl)methyloxy)-2-phenylpiperidine (360mg, 1.22mmol) in anhydrous methanol (1ml). The solvent was removed in vacuo, and the residue recrystallised from ethyl acetate-methanol to provide cis-3-((3,5- dimethylphenyl)methyloxy)-2-phenyl piperidine hydrochloride salt as a crystalline, white solid, m.p. = 200-225°C (decomp).1H NMR (360MHz, DMSO-d6)δ 7.44 (m), 6.82 (2), 6.56 (2), 4.49 (2), 4.41 (d, J = 12.3Hz), 4.09 (d, J = 12.3Hz), 3.80 (s), 3.05 (t, J = 14.7Hz), 2.14 (s), 1.90 (m), 1.72 (m); m/z (CI+) 296 (MH); Analysis: Found: C, 72.36; H, 7.91; N, 4.31. Calcd. for
C20H26NOCl; C, 72.38; H, 7.90; N, 4.22%.
EXAMPLE 3: cis-3-((3,5-Dimethylphenyl)methyloxy)-1-methyl-
2-phenylpiperidine
A solution of cis-3-((3,5-dimethylphenyl)methyloxy)-2- phenylpiperidine (220mg, 0.75mmol, Example 2) and acetic arid (0.212ml) in dry methanol (6ml) was cooled to 0°C and sodium cyanoborohydride (96mg, l.5mmol) was added followed by formaldehyde (38% aq. solution, 0.15ml). The reaction mixture was stirred at 23°C for 18h, then the solvent was removed in- vacuo and the residue partitioned between dichloromethane and 2M sodium hydroxide. The layers were separated, and the aqueous phase extracted with dichloromethane (2 x 20ml). The combined organic extracts were washed with water then brine, then dried (K2CO3) and concentrated to leave a clear oil.
Purification on silica-gel (CH2Cl2/MeOH/NH3 97:3:0.5 then CH2Cl2/MeOH 90:10) provided the title compound as a clear, colourless oil. 1H NMR (CDCI3) 7.42 (m), 7.30 (m), 6.77 (s), 6.54 (s), 4.27 (d, J = 12.2Hz), 4.04 (d, J = 12.2Hz), 3.42 (s), 3.07 (m), 2.91 (d, J = 1.9Hz), 2.17 (s), 2.10 (m) 2.04 (s), 1.56 (m), 1.39 (m).
MS (CI) m/z 310 (MH).
EXAMPLE 4: cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)- 2-phenylpiperidine hydrochloride salt
The ti tl e c o mp o un d w a s p re p a re d fro m 1 - t- butyloxycarbonyl-3-hydroxy-2-phenylpiperidine (Example 2c) and 3,5-bis(trifluoromethyl)benzylbromide in an analogous manner to that described in Example 2d,e, m.p. = 170-210°C (decomp.). 1H NMR (360MHz, DMSO)δ 7.95 (s), 7.81 (s), 7.47 (m), 7.37 (m), 4.78 (d, J = 13.3Hz), 4.56 (s), 4.32 (d, J = 13.3Hz),
3.96 (s), 3.10 (t. J = 12.7Hz), 2.23 (d, J = 13.0Hz), 2.00-1.64 (m); m/z (CI+) 404 (MH); Analysis: Found: C, 54.08; H, 4.47; N, 3.13. Calcd. for C20H20NOF6Cl.0.25H2O C, 54.06; H, 4.65; N, 3.15%.
E X A M P L E 5 : ( + ) - c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine hydrochloride salt
a) The mixture of cis- and trans-isomers of 3-hydroxy-2- phenylpiperidine (Example 2b) and 4-toluenesulfonic acid monohydrate was crystallized from methanol/ethyl acetate to give cis-3-hydroxy-2-phenylpiperidinium tosylate, m.p. 266-
267°C.
b) The tosylate salt (Example 5a) was dissolved in a mixture of ethyl acetate and 10% aqueous Na2CO3 with warming. The organic phase was washed with saturated brine, dried (K2CO3) and evaporated to give crystalline cis-3-hydroxy-2- phenylpiperidine, m.p. 110-110.5°C.
c) cis-3-Hydroxy-2-phenylpiperidine (Example 5b) and (-)dibenzoyltartrate were dissolved in methanol and crystallized by addition of ethyl acetate. The solid was recrystallised from hot methanol to give the hemi dibenzoyltartrate salt m.p. 223-
224°C. This was liberated from the salt as described above (Example 5b) to give the single enantiomer (+) cis-3-hydroxy-2- phenylpiperidine, m.p. 93-95°C. [α]23 D = +98.5° (c=1, MeOH). The mother liquors were converted to the free base as described in Example 5b and by crystallization using (+)dibenzoyltartrate in an analogous manner to that described above gave (-)cis-3- hydroxy-2-phenylpiperidine, m.p. 93-95°C. [α]23 D = -97.2° (c=1, MeOH).
d) (+) cis-3-hydroxy-2-phenylpiperidine was treated analogously to that described in Example 2c, d, e to give (+ )-cis- 3-((3,5(bis-trifluoromethyl)phenyl)methyloxy-2-phenylpiperidine hydrochloride salt, m.p. = 215-216°C. [α]23 D = 87.3° (c=1, MeOH). 1H NMR (360MHx, DMSO-d6)δ 7.95 (s), 7.81 (s), 7.47 (m), 7.37 (m), 4.78 (d, J = 13.3Hz), 4.56 (s), 4.32 (d, J = 13.3Hz), 3.96 (s), 3.10 (t, J = 12.7Hz), 2.23 (d, J = 13.0Hz), 2.00-1.64 (m); m/z (CI+) 404 (MH); Analysis: Found: C, 54.52; H, 4.60; N, 3.11. Calcd. for C20H20NOF6Cl; C, 54.62; H, 4.58; N, 3.18%. EXAMPLE 6: cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-
1-(carbomethoxy)methyl-2-phenylpiperidine
cis 3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-2- phenylpiperidine was liberated from the hydrochloride salt (Example 4, 1g) by partitioning between ethyl acetate and 2M sodium hydroxide. The organic phase was washed successively with water, saturated brine, dried (MgSO4) and evaporated in vacuo. To a solution of the residual oil in tetrahydrofuran (20ml) was added triethylamine (0.4ml) and methyl bromoacetate and the solution was heated at reflux under an atmosphere of nitrogen for 16h. To the cooled solution was added ethyl acetate and water and the organic phase washed further with water and dried (MgSO4). After the solvent had been removed in vacuo the residue was chromatographed on silica gel eluting with ethyl acetate/petroleum ether (3:10). The product which was obtained was recrystallized from diethyl ether/petroleum ether to give the title compound, m.p. =81- 83°C. Found: C, 57.35; H, 4.98; N, 2.84; C23H23F6NO3.0.1(H2O) requires C, 57.71; H, 4.86; N, 2.93%. m/z (CI+) 476 (MH).
EXAMPLE 7: cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)- 1-(carboxamido)methyl-2-phenylpiperidine
A solution of the methyl ester (Example 6, 0.6g) in methanol
(20ml) was saturated with ammonia at 0°C, sealed and stored at 5°C for 72h. The solution was evaporated to dryness and the residue chromatographed on silica gel eluting with ethyl acetate/petroleum ether (bp = 60-80°C) (1:1). The product which eluted was concentrated and recrystallized from diethyl ether/ethyl acetate to give the title compound, m.p. = 150-152°C. Found: C, 56.71; H, 4.79; N, 5.87; C22H22F6O2N2.0.1(H2O) requires C, 56.98; H, 4.80; N, 6.04%. m/z (CI+) 461 (MH), m/z (Cl-) 459 (M-H).
E X A M P L E 8 : ( + ) - c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-(carbomethoxy)methyl- 2-phenylpiperidine The title compound was prepared from (+)-cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine (Example 5) by a procedure analogous to that described in Example 6, m.p. = 60-70°C, [α]24 D = +132.3° (c=1, MeOH). Found: C, 58.31; H, 4.90; N, 2.94. C23H23F6NO3 requires C,
58.11; H, 4.88; N, 2.95%.
E X A M P L E 9 : ( + ) - c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-(carboxamido)methyl- 2-phenylpiperidinium hydrochloride
The title compound was prepared from (+)-cis-3-((3,5- Bis(trifluoromethyl)phenyl)methyloxy)-1-(carbomethoxy)methyl- 2-phenylpiperidine (Example 8) using a procedure analogous to that described in Example 7, and crystallized finally as the hydrochloride salt, m.p. = 192-3°C [α]24 D = +80.4° (c=1, MeOH).
Found: C, 53.27; H, 4.68; N, 5.56. C22H22F6O2N2.HCl requires C, 53.18; H, 4.67; N, 5.64%.
E X A M P L E 1 0 : ( + ) - c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-methyl-2- phenylpiperidine
The title compound was prepared from (+)-cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine hydrochloride (Example 5) by isolation of the free base (by extraction into ethyl acetate from 10% Na2CO3 solution) and alkylation using a procedure analogous to that described in Example 3, m.p. = 40-42°C: [α]26 D = +149° (c=0.56, MeOH); Found: C, 59.97; H, 4.95; N, 3.36. C21H21NOF6.0.1(H2O) requires C, 60.17; H, 5.10; N, 3.34%.
E X A M P L E 1 1 : ( - ) - c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine hydrochloride salt
The title compound was prepared from (-)-cis-3-hydroxy-2- phenyl piperidine (Example 5c) by a procedure analogous to that described in Example 5d, m.p. = 215-216°C. [α]D 23 = -86.9° (c=1, MeOH). Found: C, 54.44; H, 4.54; N, 3.11. Calcd for
C20H19NOF6.HCl; C, 54.62; H, 4.58; N, 3.18%.
EXAMPLE 12: trans-((3,5-Dimethylphenyl)methyloxy)-2-phenyl piperidine hydrochloride salt
The title compound was prepared from trans-1-t-butyloxy carbonyl-3-hydroxy-2-phenylpiperidine (Example 2c) by a procedure analogous to that described in Example 2d, e, m.p. = 210-235°C. E X A M P L E 1 3 : t r a n s - 3 - ( ( 3 , 5 -
Bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine hydrochloride salt
The title compound was prepared in an analogous manner to that described in Example 4 and separated from the cisisomer by chromatography on silica gel and crystallisation as the hydrochloride salt, m.p. = 216-226°C. Found: C, 54.38; H, 4.54; N, 3.12. Calcd for C20H19NOF6.HCl; C, 54.62; H, 4.58; N, 3.18%.
E X A M P L E 14 : ( 2 S , 3 S ) - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1,1-dimethyl-2-phenyl piperidinium iodide
The title compound was prepared from the N-methyl amine (0.24g, Example 10) with methyl iodide (0.178ml) in diethyl ether (3ml). After 62h the white solid which formed was isolated by filtration and washed with ether, m.p. = 204-205°C.
Found: C, 46.74; H, 4.29; N, 2.41. Calcd for C22H24NOF6I.0.3H2O; C, 46.79; H, 4.39; N, 2.48%.
EXAMPLE 15: (2S,3S)-1-Acetyl-3-((3,5-bis(trifluoromethyl) phenyl)methyloxy)-2-phenyl piperidine
To a solution of (+)-cis-3-((3,5-bis(trifluoromethyl) phenyl)methyloxy)-2-phenyl piperidine prepared from hydrochloride salt (Example 5, 1.0g) by partitioning between aqueous sodium carbonate and dichloromethane) in dry dichloromethane (5ml) was added pyridine (0.67ml), acetic anhydride (0.79ml) and 4,4-dimethylamine pyridine (10mg). After the solution had been stirred for 3h at 23°C, saturated sodium bicarbonate solution was added and the organic phase dried (MgSO4), evaporated in vacuo and chromatographed on silica gel to give the title compound as an oil. Found: C,59.51;
H, 4.90; N, 3.09. Calcd for C22H21NO2F6; C, 59.33; H, 4.75; N, 3.14%. EXAMPLE 16: (2S,3S)-1-Formyl-3-((3,5-bis(trifluoromethyl) phenyl)methyloxy)-2-phenyl piperidine
The title compound was prepared from (+)-cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine (prepared from the hydrochloride salt, Example5 )(0.5g) and formic-acetic anhydride (prepared from 90% formic acid (1.0ml) and acetic anhydride (3ml) at 60°C for 30 minutes) in tetrahydrofuran for 48h at 23°C. The solvent was evaporated in υacuo and the residue partitioned between diochloromethane and saturated aqueous sodium bicarbonate solution, dried
(MgSO4), concentrated in vacuo and chromatographed on silica gel to give the title compound as an oil. Found: C,57.79; H,
4.39; N, 3.13. Calcd for C21H19NO2F6.0.3(H2O), C,57.75; H,
4.52; N, 3.21%.
EXAMPLE 17: (2S,3S)-1-Benzyl-3-((3,5-bis(trifluoromethyl) phenyl)methyloxy)-2-phenylpiperidine
Benzyl bromide (0.134ml) was added to a mixture of (+)-cis- 3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine (prepared from the hydrochloride salt, Example5 ) 0.5g) and potassium carbonate (0.468g) in N,Ndimethylformamide (2ml) and the mixture stirred at 23°C for 2.5h. Water (20ml) was added and the mixture extracted with ethyl acetate (3 x 15ml). The combined organic extracts were washed with water (1 x 10ml) and brine (1 x 10ml) then dried (K2CO3) and concentrated to leave an oil. Purification on silica gel eluting with hexanes-ethyl acetate (19:1 then 9:1 then 4:1 then 1:1) provided the title compound as a solid, m.p. = 89-93°C. Found: C, 66.11; H, 5.25; N, 2.81. Calcd. for C27H25NOF6; C, 65.71; H, 5.11; N, 2.84%.
E X A M P L E 1 8 : ( 2 S , 3 S ) - 3 - ( 3 , 5 -
Bis(trifluoromethyl)phenyl)methyloxy)-1-(1-carbomethoxy)ethyl- 2-phenyl piperidine
The title compound was prepared in a manner analogous to that described in Example 17 with methyl DL-2- bromopropionate and potassium carbonate in N,Ndimethylformamide at 80°C for 2h. Purification by chromatography on silica gel provided diastereoisomer A as a solid, m.p. = 65-66°C. Found: C,58.87; H, 5.12; N, 2.94. Calcd for C24H25NO3F6; C, 58.89; H, 5.15; N, 2.86%, and diastereoisomer B as an oil, 1H NMR (360MHz, CDCI3)δ 7.7 (s),
7.5 (m), 7.3 (m), 4.45 (d), 4.06 (d), 3.77-3.47 (m), 3.06 (br d), 2.59 (t), 2.10 (m), 1.54 (m), 1.03 (d), m/z (CI+) 490 (MH).
E X A M P L E 1 9 : ( 2 S , 3 S ) - 3 - ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-(carboxamido)ethyl-2- phenylpiperidinium hydrochloride
A solution of the methyl ester (diastereoisomer B, Example
18) in methanol was added to liquid ammonia at -50°C then heated to 150°C (60 Bar) for 48h. The solution was evaporated to dryness and the residue chromatographed on silica gel eluting with hexanes/ethvl acetate (4:1) then ethyl acetate/methanol (9: 1). The title compound was crystallised finally as the hydrochloride salt, m.p. = 112-117°C.
EXAMPLE 20: cis-3-(3,5-Bis(trifluoromethyl)phenyl)methyloxy- 6-methyl-2-phenyl piperidinium hydrochloride
Magnesium metal (1.03g, 42.8mmol), 6ml of a solution of 4- bromo-1-butene (5.5g, 40.8mmol) in dry tetrahydrofuran (30ml) and 1,2-dibromoethane (2 drops) were gently warmed until reaction commenced. The remainder of the bromoalkene solution was then added dropwise over 10 min. The reaction mixture was stirred at 23°C for 1h, then added to a cooled (- 10°C) solution of N-Boc phenyl glycine aldehyde (3.2g) in dry tetrahydrofuran (20ml), the mixture was allowed to warm to 23°C, stirred for 1h then quenched by the addition of saturated aqueous ammonium chloride solution. The layers were separated, the aqueous phase was extracted with ethyl acetate (3 x 60ml), the combined organic phases were washed with brine (1 x 5 0ml), dried (MgSO4) and concentrated to leave N-Boc-2- hydroxy-1-phenyl-hex-5-enyl-1-amine as a pale yellow oil. 1H NMR (250MHz, CDCI3) δ 7.4-7.2 (m), 5.9-5.7 (m), 5.35 (d), 5.1-
4.9 (m), 4.65 (br m), 3.85 (m), 2.2 (m), 1.65 (m), 1.45 (s).
Sodium hydride (80% in oil, 161mg) was added to a solution of N-Boc-2-hydroxy-1-phenyl-hex-51enyl-1-amine (1.2g) and 3,5- bis-trifluoromethylbenzylbromide ( 1.13ml) in dry N,Ndimethylformamide (5ml). The reaction mixture was stirred for 16h at 23°C, then diluted with water (50ml) and extracted with ethyl acetate (3 x 40ml). The combined organic phases were washed with water (1 x) and brine (1 x) then dried (MgSO4) and concentrated to leave an oil. Purification by chromatography on silica gel (hexanes/ethyl acetate 9:1 then 4:1 then 1:1) provided
N-Boc-2-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-phenylhex-5-enyl-1-amine as a pale yellow oil. 1H NMR (360MHz, CDCl3) 57.78 (s), 7.72 (s), 7.35-7.25 (m), .752 (m), 4.95 (m), 4.65 (d), 4.50 (d), 4.05 (d), 3.60 (q), 2.11 (m), 1.66 (m).
A solution of N-Boc-2-((3,5-bis(trifluoromethyl)phenyl) methyloxy)-1-phenyl-hex-5-enyl-1-amine (0.3g) and mercuric acetate (0.37g) in dry tetrahydrofuran (6ml) was stirred at 50°C under N2 for 15h. The solvent was removed in vacuo and the residue dissolved in chloroform (20ml) and mixed thoroughly with saturated potassium chloride solution (10ml). The layers were separated, and the aqueous phase extracted with chloroform (1 x 15ml). The combined organic phases were dried (MgSO4) and concentrated to leave a yellow oil.
The cru de p r o d uc t w a s di s s o lv e d i n dry N , Ndimethylformamide (2ml) and added dropwise to a stirred suspension of sodium borohydride (0.042mg, llmmol) in dry N,N-dimethylformamide. The reaction mixture was stirred for 0.5h at 23°C then diluted with diethyl ether and filtered through a pad of Hi-flo. The filtrate was poured into water (30ml) and extracted with ethyl acetate (3 x 20ml). The combined organic extracts were washed with saturated aqueous sodium bi carbonate solution (1 x 15ml) and brine (1 x 15ml) then dried (MgSO4) and concentrated to leave an orange-yellow oil. Purification by chromatography on silica gel eluting with hexanes/ethyl acetate (19:1) provided 3-((3,5- bis(trifluoromethyl)phenyl)methyloxy-1-(t-butyloxycarbonyl)-6- methyl-2-phenylpiperidine as a clear, viscous oil.
This material was dissolved in trifluoroacetic acid (2ml) under nitrogen, after 10 min the trifluoroacetic acid was evaporated in vacuo and the residue partitioned between 2M sodium hydroxide and dichloromethane. The layers were separated, and the aqueous phase extracted with dichloromethane (2 x 20ml). The combined organic phases were dried (K2CO3) and concentrated to leave an oil, which was purified by chromatography on silica gel eluting with hexanes/ethyl acetate (4:1 then 1:1) to provide 3-((3,5- bis(trifluoromethyl)phenyl)methyloxy-6-methyl-2-phenyl piperidine as a clear, viscous oil. The title compound was finally crystallised as the hydrochloride salt, m.p. = 218-220°C. Found: C,55.15; H, 4.79; N, 3.33; Calcd. for C21H22NOClF6 C, 55.55; H, 4.89; N, 3.09%.
E X A M P L E 2 1 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-2-(2- chlorophenyl)piperidine
a) Methyl-4-nitrobutyrate and 2-chlorobenzaldehyde were reacted in an analogous manner to that described in Example 2a to give 6-(2-chlorophenyl)-5-nitro-2-oxopiperidine. 1H NMR (360MHz, CDCI3)δ 2.00-2.18 (1H, m), 2.42-2.61 (3H, m), 4.80- 4.87 (1H, m), 5.91 (1H, d), 6.41 (1H, s), 7.17-7.42 (4H, m).
b) Sodium methoxide (0.25g) was added to a suspension of 5-nitro-2-oxo-6-(2-chlorophenyl)piperidine (1.0g) in methanol (10ml) to give solution (A).
To a cooled (0°C) solution of ammonium acetate (9.61g,
125mmol) in degassed water (30ml) under nitrogen was added titanium trichloride ( 13% solution in 20% HCl, 29.6ml, 23.4mmol) over 20 min. Solution (A) was added over 20 min. The resulting mixture was stirred at 23°C for 2 hrs, then extracted with ethyl acetate (150ml x 4). The combined organic extracts were washed with brine (40ml), then dried (MgSO4) and concentrated to give 6-(2-chlorophenyl)-2,5-dioxopiperidine. 1H NMR (250MHz, CDCl3) δ 2.81-2.93 (4H, m), 5.4 (1H, m), 5.8 (1H, s), 7.20-7.40 (4H, m).
c) To a stirred suspension of 6-(2-chlorophenyl)-2,5- dioxopiperidine (2.50g) in methanol (25ml) under nitrogen at -30°C was added, portionwise, sodium borohydride (0.21g). After 10 min HPLC indicated no starting material remained. The mixture was concentrated in vacuo and the residue azeotroped with toluene (2 x 30ml). The crude material was cooled (0°C) and borane-tetrahydrofuran complex (45ml, 1.0M solution in tetrahydrofuran) was added over 25 min. When the addition was complete the mixture was heated at reflux for 16 hrs. The reaction mixture was cooled to 5°C and quenched with methanol, then concentrated in vacuo. The residue was dissolved in ethanol (30ml) and potassium carbonate (3.10g) was added and the mixture was heated at reflux for 6 hrs. The solvent was removed in vacuo and the residue was partitioned between ethyl acetate (50ml) and water (100ml). The aqueous layer was extracted with ethyl acetate (3 x50ml). The combined organic extracts were dried (MgSO4) and concentrated in vacuo. Η NMR (360MHz, DMSO) δ 51.66-1.70 (1H, m), 1.82-2.12 (3H, m), 2.28 (3H, s), 3.31 (1H, m), 4.04 (1H, s), 4.64 (1H, d), 5.6 (1H, s), 7.08 (2H, d), 7.4-7.61 (6H, m). The residue was dissolved in methanol (20ml) and p-toluene sulphonic acid (2.13g) was added. Evaporation in vacuo and recrystallisation from ethyl acetate/methanol gave cis-2-(2-chlorophenyl)-3- hydroxypiperidine tosylate salt.
d) The product of part c) was dissolved in a mixture of dichloromethane and 10% aqueous sodium carbonate solution with gentle warming. The organic phase was washed with saturated brine, dried (MgSO4) and concentrated to give cis-2-
(2-chlorophenyl)-3-hydroxypiperidine. Di-t-butyldicarbonate was added to cis-2-(2-chlorophenyl)-3-hydroxypiperidine in an analogous manner to that described in Example 2c to give cis-1- t-butyloxycarbonyl-2-(2-chlorophenyl)-3-hydroxypiperidine. 1H NMR (250MHz, CDCl3) δ 51.24 (9H, s), 1.40-2.10 (4H, m), 3.40-
3.56 (1H, m), 4.08-4.22 (1H, m), 4.26-4.36 (1H, m),5.40 (1H, d), 7.18-7.42 (4H, m).
e) The product of part d) and 3,5-bis( trifluoromethyl)benzyl bromide were added together in an analogous manner to that described in Example 2d to give cis 3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-t-butyloxycarbonyl-2- (2-chlorophenyl)piperidine. 1H NMR (360MHz, CDCI3) δ 1.22 (9H, s), 1.62-2.20 (4H, m), 3.38-3.47 (1H, ddd), 4.16-4.20 (2H, m), 4.21-4.25 (1H, d), 4.46-4.50 (1H, d), 7.13-7.38 (4H, m), 7.40 (2H, s), 7.64 (1H, s). m/z (CI+) 538, 540.
f) The product of part e) was treated with trifluoroacetic acid in an analogous manner to that described in Example 2e and crystallised as the oxalate salt, m.p. = 165°C. 1H NMR (360MHz, DMSO-d6)δ 1.64-1.92 (3H, m), 2.21-2.30 (1H, m), 3.20-3.42 (2H, m), 4.00 (1H, s), 4.30-4.34 (1H, d), 4.78-4.80 (1H, d), 4.80-4.84 (1H, s), 7.38-7.40 (2H, m), 7.45-7.51 (1H, m), 7.57-
7.61 (1H, m), 7.75 (2H, s), 7.94 (1H, s). Found: C, 48.57; H, 3.92; N, 2.51. C20H18ClF6NO.C2O4H2.H2O requires: C, 48.41; H, 4.06; N, 2.57%. E X A M P L E 2 2 : c i s - 3 - ( ( 3 , 5 -
Bis(trifluoromethyl)phenyl)methyloxy)-2-(3- chlorophenyDpiperidine hydrochloride salt
a) Methyl-4-nitrobutyrate and 3-chlorobenzaldehyde were reacted in an analogous manner to that described in Example 2a to give 2-(3-chlorophenyl)-3-nitro-6-oxopiperidine, m.p. = 131-
133°C.1H NMR (360MHz, CDCI3) δ 2.26-2.36 (1H, m), 2.50-2.72 (3H, m), 4.66-4.71 (1H, m), 5.24-5.28 (1H, d), 6.57 (1H, s), 7.17- 7.40 (4H, m).
b) The product of part a) was treated analogously to that described in Example 2b to give 2-(3-chlorophenyl)-3,6-dioxo piperidine, m.p. = 144-147°C. 1H NMR (250MHz, CDCI3) 52.8 (4H. m), 5.0 (1H, d), 6.4 (1H. s., 7.22-7.42 (4H, m). c) The product of part b) was treated analogously to that described in Example 21c to give cis-2-(3-chlorophenyl)-3- hydroxypiperidine tosylate salt, m.p. > 250°C.1H NMR (250MHz, DMSO-d6) δ 1.60-2.07 (4H, m), 2.28 (3H, s), 3.00-3.11 (1H, m), 4.02 (1H, s), 4.62-4.66 (1H, d),5.96 (1H, s), 7.10-7.20
(2H, d), 7.41-7.59 (6H, m).
d) The product of part c) was treated analogously to that described in Example 2 Id to give cis- 1-t-butyloxycarbonyl-2-(3- chlorophenyl)-3-hydroxypiperidine as a clear, viscous oil. 1H NMR (360MHz, CDCl3) δ 1.40 (9H, s), 1,61-1.90 (4H, m), 2.88-
3.01 (1H, ddd), 3.93-3.99 (1H, dd), 4.03-4.10 (1H, m), 5.33 (1H, d), 7.20-7.26 (2H, m), 7.34-7.38 (1H, m), 7.47-7.52 (1H, m). m/z (CI-) 310, 312; m/z (CI+) 312, 314.
e) The product of part d) and 3,5- bis(trifluoromethyl)benzylbromide were treated in an analogous manner to that described in Example 2d to give cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-t-butyloxycarbonyl-2- (3-chlorophenyl)piperidine. 1H NMR (250MHz, CDCI3) δ 1.24- 1.30 (1H, m), 1.47 (9H, s), 1.60-2.00 (3H, m), 2.67-2.80 (1H, ddd), 3.81-4.01 (2H, m), 4.8 (2H, s),5.61-5.67 (1H, d), 7.23-7.27 (2H, m), 7.39-7.44 (1H, m), 7.6 (1H, s), 7.78 (2H, s), 7.8 (1H, s).
f) The product of part e) was treated in an analogous manner to that described in Example 2e to give cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-(3- chlorophenyl)piperidine hydrochloride salt, m.p. = 158°C.1H NMR (360MHz, DMSO-d6)δ 1.70-1.96 (4H, m), 2.19-2.28 (1H, m), 3.02-3.13 (1H, m), 3.84 (1H, s), 4.35-4.39 (2H, d), 4.60 (1H, s), 4.79-4.85 (2H, d), 7.39-7.44 (3H, m), 7.58 (1H, s), 7.84 (2H, s), 7.97 (1H, s), 9.2 (br s), 10.05 (br s). Found: C,50.44; H, 4.13; N,
3.01. C20H18ClF6NO.HCl requires C,50.65; H, 4.04; N, 2.95%. m/z (CI+), 438, 440.
E X A M P L E 2 3 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-2-(4- chlorophenyl)piperidine hydrochloride salt
a) Methyl-4-nitrobutyrate and 4-chlorobenzaldehyde were treated in an analogous manner to that described in Example 2a to give 2-(4-chlorophenyl)-3-nitro-6-oxopiperidine. 1H NMR (360MHz, CDCl3)δ 2.24-2.38 (1H, m), 2.61-2.70 (3H, m), 4.60-
4.69 (1H, m), 5.20 (1H, d), 6.82 (1H, s), 7.22-7.26 (2H, d), 7.36- 7.40 (2H, d).
b) The product of part a) was treated in an analogous manner to that described in Example 2b to give 2-(4- chlorophenyl)-3,6-dioxopiperidine. 1H NMR (260MHz, CDCI3) δ
2.8 (4H, s), 5.0 (1H, d), 6.4 (1H, s), 7.22-7.46 (4H, q).
c) The product of part b) was treated analogously to that described in Example 21c to give cis-2-(4-chlorophenyl)-3- hydroxypiperidine tosylate salt.1H NMR (360MHz,-DMSO-d6)δ 1.62-2.13 (4H, m), 2.30 (3H, s), 3.01-3.26 (2H, m), 4.00 (1H, s),
4.28 (1H, s),5.00-5.60 (b), 7.11-7.15 (2H, d), 7.44-7.56 (6H, m), 8.60-9.10 (b). d) The product of part c) was treated analogously to that described in Example 21d to give cis-1-t-butyloxycarbonyl-2-(4- chlorophenyl)-3-hydroxypiperidine, m.p. = 95-96°C, m/z (CI+) 312, 314.
e) The product of part d) (0.7g, 2.25mmol) was dissolved in ethylene glycol dimethyl ether (1ml). 0.5M potassium bis(trimethylsilyl)amide (4.9ml) was added. The mixture was stirred at 23°C for 20 min, then 3,5- bis(trifluoromethyl)benzylbromide (0.50ml) was added. After stirring for 18 hr the solvent was removed in vacuo, and the residue partitioned between ethyl acetate and water. The organic phase was dried (MgSO4). The residue after removal of solvent in vacuo, was chromatographed on silica gel using hexane/ethyl acetate (9:1) as eluant to give cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-t-butyloxycarbonyl-2-
(4-chlorophenyl)piperidine, 1H NMR (360MHz, CDCI3) δ 1.46 (9H, s), 1.68-2.04 (4H, m), 2.66-2.76 (1H, ddd), 3.82-3.98 (2H, m), 4.72 (2H, s), 6.64 (1H, s), 7.28-7.32 (2H, d), 7.46-7.60 (2H, d), 7.70 (2H, s), 7.80 (1H, s). m/z (CI+) 438, 640.
f) The product of part e) was dissolved in diethyl ether
(5ml). Saturated hydrogen chloride in diethyl ether (10ml) was added. The mixture was stirred at 23°C under nitrogen for 2.5 hrs, then concentrated in vacuo. Recrystallisation from ethyl acetate/diethyl ether provided cis-3-(3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-(4- chlorophenyl)piperidine hydrochloride salt, m.p. = 202°C. 1H NMR (360MHz, DMSO-d6)δ 1.65-1.96 (3H, m), 2.20-2.26 (1H, m), 3.02-3.14 (1H, ddd), 3.21-3.37 (1H, m), 3.94 (1H, s), 4.36-4.42 (1H, d), 4.6 (1H, s), 4.78-4.80 ( 1H, d), 7.40-7.47 (4H, m), 7.78 (2H, s), 8.00 (1H, s). m/z (CI+) 438, 446. Found: C, 48.97; H, 3.98; N, 2.80. C20H19Cl2F6NO.H2O, requires C, 48.79; H, 4.29; N, 2.84.
EXAMPLE 24: cis-3-(3,5-Bis(trifluoromethyl)phenyl)methyloxy)- 2-(4-methylphenyl)piperidine hydrochloride salt a) Methyl-4-nitrobutyrate and 4-methylbenzaldehyde were treated in an analogous manner to that described in Example 2a to give 2-(4-methylphenyl)-3-nitro-6-oxopiperidine. 1H NMR (360MHz, CDCl3) δ 2.4 (3H, s), 2.47-2.65 (4H, m), 4.62-4.67 (1H, m), 5.2 (1H, d), 6.11 (1H, s), 7.2 (4H, q).
b) The product of part a) was treated in an analogous manner to that described in Example 2b to give 2-(4- methylphenyl)-3,6-dioxopiperidine. NMR (360MHz, CDCI3) δ 2.17 (3H, s), 2.24-2.81 (4H, m), 4.9 (1H, d), 6.2 (1H, s), 7.21 (4H, q) .
c) The product of part b) was treated analogously to that described in Example 21c to provide cis-2-(4-methylphenyl)-3- hydroxypiperidine tosylate salt. 1H NMR (free base, 250MHz, CDCI3) δ 1.21-1.43 (2H, m), 1.60-1.83 (2H, m), 2.13 (3H, s), 2.47- 2.65 (1H, ddd), 3.01 (1H, m), 3.57 (1H, s), 3.83 (1H, s), 7.00-7.20
(4H, q). d) The product of part c) was treated analogously to that described in Example 2d to give cis-1-t-butyloxycarbonyl-3- hydroxy-2-(4-methylphenyl)piperidine. 1H NMR (360MHz, CDCl3)δ 1.27 (9H, s), 1.61-1.80 (4H, m), 2.11 (3H, s), 2.91-2.99 (1H, ddd), 3.91-4.01 (2H, m), 5.22 (1H, d), 7.02 (2H, d), 7.16 (2H, d). m/z (CI+) 292.
e) The product of part d) was treated in an analogous manner to that described in Example 23e to give cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-t-butyloxycarbonyl-2- (4-methylphenyl)piperidine. 1H NMR (250MHz, CDCI3) δ 1.41
(9H, s), 1.60-1.69 (2H, m), 7.89-2.01 (2H, m), 2.17 (3H, s), 2.65- 3.03 (1H, ddd), 3.87-3.99 (2H, m), 4.74 (2H, q), 5.71 (1H, d), 7.10 (2H, d), 7.21 (2H, d), 7.65 (2H, s), 7.81 (1H, s).
f) cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-1-t- butyloxycarbonyl-2-(4-methylphenyl)piperidine was treated analogously to that described in Example 23f to give cis-3-(3,5- bis(trifluoromethyl)phenyl)methyloxy-2-(4- methylphenyl)piperidine hydrochloride salt, m.p. = 195°C.1H NMR (360MHz, DMSO-d6)δ 1.62-1.96 (4H, m), 2.13 (3H, s), 3.01-3.12 (1H, ddd), 3.91 (1H, s), 4.26 (1H, d), 4.47 (1H, s), 4.80
(1H, d), 7.20 (2H, d), 7.31 (2H, d), 7.80 (2H, s), 7.92 (1H, s). Found: C, 53.22; H, 4.76; N, 2.93. C21H21F6NO.1.5HCl requires C, 63.43; H, 4.80; N, 2.97%. m/z (CI+) 418. E X A M P L E 2 5 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-2-thienyl piperidine hydrochloride salt
a) Thiophene-2-carboxaldehyde (9.26ml), methyl-4- nitrobutyrate ( 12.81ml) and ammonium acetate (10.01g) were added to ethanol (140ml) and then the reaction mixture was refluxed for 3h. The reaction was cooled to room temperature and ethanol was removed in vacuo. Ethyl acetate was added to the residue and insoluble material was filtered off. This afforded 5-nitro-2-oxo-6-thienylpiperidine as a yellow crystalline solid. 1H NMR (250MHz, DMSO) δ 2.15-2.33 (2H, m, CH2), 2.34 (2H, m, CH2), 5.10-6.21 ( 1H, m, CHNO2), 5.36-5.46 ( 1H, m, NCH), 6.28-6.37 (1H, brs, NH), 7.01-7.14 (2H, m, ArH), 7.52-7.58 (1H, m, ArH).
b) A 13% solution of titanium trichloride in 20% hydrochloric acid (173ml) was added to a degassed solution of ammonium acetate (100g) in methanol (300ml) at 0°C under nitrogen over 20 min. A solution of sodium methoxide (1.49g) in methanol (60ml) was added to a suspension of 5-nitro-2-oxo-6- thienylpiperidine (5g, Example 25a) in methanol (75ml) and the mixture stirred for 20 min. This solution was then added dropwise to the titanium trichloride/buffer solution at 0°C under nitrogen. The reaction was stirred at 0°C for 30 min and at 23°C for 30 min. Methanol was removed in vacuo and ethyl acetate was added to the residue. The emulsion was filtered through Hi-flo and then shaken with brine. The organic phase was dried (MgSO4) and concentrated in vacuo. The material was chromatographed on silica using (1: 1 then 9: 1) ethyl acetate in petroleum ether (60-80) as eluant to give 2,5-dioxo-6- thienylpiperidine. m/z (CI+) m/z 105 (MH, 53%).
c) 2,5-Dioxo-6-thienylpiperidine (1.16g, Example 25b) was suspended in methanol (40ml) under nitrogen. The temperature was maintained at -40°C using an acetonitrile/dry ice bath while sodium borohydride (0.11g) was added portionwise. The reaction mixture was allowed to warm to room temperature and then stirred for lh. Methanol was removed in vacuo and the material was azeotroped with toluene. Borane-tetrahydrofuran complex (1.0M solution) (23.8ml) was added at room temperature and the reaction mixture was reflux ed for 3h. The reaction mixture was cooled and quenched carefully with methanol before removing the solvent in vacuo. Ethanol (60ml) was added followed by potassium carbonate (1.64g) and the reaction mixture was refluxed for 18h. The solvent was removed in vacuo. 1M Sodium hydroxide solution (30ml) and dichloromethane (30ml) were added to the residue followed by di-t-butyldicarbonate (2.25g). After stirring for 7h the organic layer was separated and concentrated in vacuo. The product, cis-1-t-butyloxycarbonyl-3-hydroxy-2-thienylpiperidine, was recrystallised from hexane, m/z (CI+) 283 ((MH), 82%).
d ) cis-1-(t-Butyloxγcarbonyl)-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-thienylpiperidine was prepared from cis-1-t-butyloxycarbonyl-3-hydroxy-2- thienylpiperidine (0.97g, Example 25c) and 3,5- bis(trifluoromethyl)benzyl bromide (0.94ml) in an analogous manner to that described in Example 2d. The material was purified by chromatography on silica using 20% ethyl acetate in petroleum ether (60-80) as eluant. 1H NMR (250MHz, CDCI3)δ 1.49 (9H, s, CH3), 1.54-2.05 (4H, m, CH2), 2.87 (1H, dt, NCHH),
3.75-3.85 (1H, m, NCHH), 3.97 (1H, brd, CHO), 4.71 (1H, d, OCHH), 4.85 (1H, d, OCHH), 5.95 (1H, brs, NCH), 6.98-7.03 (1H, m, thienyl H), 7.05-7.09 (1H, m, thienyl H), 7.24-7.30 (1H, m, thienyl H), 7.80 (3H, s, aromatic H).
e) The trifluoroacetate salt of cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-thienylpiperidine was prepared from cis-1-t-butyloxycarbonyl-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-thienylpiperidine in an analogous manner to that described in Example 2e. The material was partitioned between 10% sodium hydroxide and ethyl acetate. The layers were separated and the aqueous phase was extracted twice with ethyl acetate. The combined organic phases were dried (Na2SO4) and concentrated to give cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-thienylpiperidine.
A saturated solution of acetyl chloride in methanol was added to a s o l uti on of ci s-3-( ( 3 ,5- bis(trifluoromethyl)phenyl)methyloxy)-2-thienylpiperidine in methanol. The solvent was removed in vacuo and the residue recrystallised from diethyl ether-methanol to provide cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-thienyl piperidine hydrochloride as a white crystalline solid. 1H NMR (360MHz, DMSO) δ 1.65-1.93 (3H, m, CH2CHH), 2.21-2.29 (1H, m, CHH), 3.06-3.14 (1H, m, NCHH), 3.20-3.29 (1H, d, NCHH), 4.00 (1H, br s, CHO), 4.61 ( 1H, d, J = 13.1Hz, OCHH), 4.90 ( 1H, d, J = 13.1Hz, OCHH), 7.07 (1H, dd, thienyl H), 7.29-7.33 (1H, m, thienyl H), 7.58-7.62 (1H, m, thienyl H), 8.02 (1H, s, ArH), 8.11 (2H, s, ArH).
E X A M P L E 2 6 : ci s - 3- (( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-2-pyridyl piperidine dihydrochloride salt
a) Methyl-4-nitrobutyrate ( 12.81ml), ammonium acetate (10.01g) and freshly distilled pyridine-2-carboxaldehyde were added to ethanol (140ml) and the reaction mixture was stirred at room temperature under nitrogen for 1.5h before being heated to reflux for 45 min. The reaction mixture was allowed to cool and left for 24h. The brown crystals which formed were filtered off and in this way 4-nitro-2-oxo-5-pyridylpiperidine was isolated together with some residual ammonium acetate. 1H
NMR (260MHz, CDCI3) δ 2.15-2.32 (2H, m, CH2), 2.47-2.69 (H, m, CH2 + acetate), 5.19-6.28 (1H, m, CHNO2), 5.43-6.49 (1H, m, NCH), 6.70 (1H, brs, NH), 7.27-7.34 ( 1H, m, ArH), 7.38-7.44 (1H, m, ArH), 7.74-7.84 (1H, m, ArH), 8.60-8.67 (1H m, ArH). b ) A 13% solution of titanium trichloride in 20% hydrochloric acid (143ml) was added to a degassed solution of ammonium acetate (56g) in water (200ml) at 0°C under nitrogen over 30 min. A solution of potassium t-butoxide ( 1.91g) in methanol (40ml) was added to a solution of 4-nitro-2-oxo-5- pyridylpiperidine (3.01g, Example 26a) in methanol (65ml) and the mixture was stirred for 15 min. This solution was then added dropwise to the titanium trichloride/buffer solution at 0°C under nitrogen. The reaction mixture was stirred at 0°C for 15 min. Methanol was removed in vacuo and solid sodium hydroxide was added, with stirring and cooling, to the residual solution. The mixture was filtered and water was removed from the filtrate in vacuo. The residue was azeotroped with toluene and then redissolved in dichloromethane. Insoluble material was filtered off and the filtrate was concentrated in vacuo. The material was freeze-dried for 18h to give 5-hydroxy-2-oxo-6- pyridylpiperidine as a mixture of cis and trans isomers. 1H NMR (250MHz, CDCl3) δ 1.91-2.18 (2H, m, CH2), 2.39-2.57 (1H, m, CHH), 2.60-2.84 ( 1H, m, CHH), 4.02-4.11 (0.4H, CHOH, trans isomer), 4.37-4.44 (0.6H, m, CHOH, cis isomer), 4.61 ( 0.4H, brd, NCH , trans isomer), 4.69 ( 0.6H, brd, NCH, cis isomer), 7.30-7.50 (2H, m, ArH), 7.77-7.88 ( 1H, m, ArH), 8.54- 8.64 (1H, m, ArH).
c) 5-Hydroxy-2-oxo-6-pyridylpiperidine (2.19g, Example 26b) was dissolved in tetrahydrofuran (50ml) at room temperature under nitrogen. Borane-tetrahydrofuran complex ( 1.0M solution) (79.8ml) was added and the reaction mixture was refluxed for 23h. The reaction was allowed to cool and was quenched carefully with methanol before removing the solvent in vacuo. 6N Hydrochloric acid (50ml) was added and the mixture was stirred for 45 min. The solvent was removed in vacuo and the residue was redissolved in methanol-water. The solution was basified with solid sodium hydroxide. Di-t-butyldicarbonate (4.23g) was added and the reaction mixture was stirred for 18h. Methanol was removed in vacuo and the product was extracted into ethyl acetate. The organic phase was dried (MgSO4) and concentrated. The material was purified by chromatography on silica using 50% ethyl acetate in petroleum ether (60-80) as eluant to give cis-1-t-butyloxy-carbonyl-3- hydroxy-2-pyridylpiperidine. 1H NMR (250MHz, CDCl3) δ 1.35- 1.52 (9H, CH3), 1.60-1.84 (3H, m, CH2CHH), 1.86-2.08 (1H, m, CHH), 2.87-3.01 (1H, m, NCHH), 3.99-4.13 (1H, m, NCHH), 4.69-4.77 (1H, m, CHOH), 5.24-5.31 (1H, br d, NCH), 7.13-7.22
(2H, m, ArH), 7.63-7.73 (1H, m, ArH), 8.52-8.60 (1H, m, ArH). d ) cis-1-t-Butyloxycarbonyl-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-pyridylpiperidine was prepared from cis-1-t-butyloxycarbonyl-3-hydroxy-2- pyridylpiperidine (375mg, Example 26c) and 3,5- bis(trifluoromethyl)benzyl bromide (0.37ml) in an analogous manner to that described in Example 2d. The material was purified by chromatography on silica using 10% then 20% ethyl acetate in petroleum ether (60-80) as eluant. MS (CI+) m/z 504 (MH, 100%).
e) cis-1-t-Butyloxycarbonyl-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-pyridylpiperidne (210mg, Example 26d) was dissolved in methanol (5ml) with stirring. A saturated solution of acetyl chloride in methanol was added and the mixture stirred for 2.6h. Solvent was removed in vacuo and the material was recrystallised from diethyl ether- methanol to provide the title compound as a white crystalline solid. Η NMR (360MHz, DMSO)δ 1.56-1.69 (1H, m, CHH), 1.81-2.02 (2H, m, CH2), 2.38-2.47 (1H, m, CHH), 2.97-3.10 (1H, m, NCHH), 3.24 (1H, brd, NCHH), 3.74-3.84 (1H, m, CHO), 4.29-4.48 (2H, m, NCH and OCHH), 4.72 (1H, d, J = 13.1Hz, OCHH), 7.43-7.50 (1H, m, ArH), 7.56 (3H, brs, ArH), 7.83-7.89
(1H, m, ArH), 7.94 (1H, s, ArH), 8.57-8.62 (1H, m, ArH); MS (CI+) m/z 404, (MH, 100%).
E X A M P L E 2 7 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-6-keto-1-(4- methoxybenzyl)-2-phenyl piperidine
a) cis-3-(t-Butyldimethylsilyloxy)-6-keto-2-phenyl piperdine Sodium borohydride (2g) was added to a cooled (-10°C) suspension of 3,6-diketo-2-phenylpiperidine (20g, Example 2b) in methanol (300ml) with stirring. After O.5h the solvent was removed in vacuo, and the residue dissolved in water (100ml), then neutralised (pH 7, acetic acid) and extracted with ethyl acetate (3 x 100ml). The combined organic phases were dried (K2CO3) and concentrated to leave a white solid. A further batch was obtained by continuous extraction of the aqueous layer with ethyl acetate.
This material was suspended in dichloromethane (200ml), cooled to 0°C and 2,6-lutidine (13ml) was added followed by t- butyldimethylsilyl trifluoromethanesulfonate (25.5ml). The resultant pale yellow solution was stirred at 23°C for 5h, then poured into saturated aqueous sodium bicarbonate solution (200ml), the layers were separated and the aqueous phase extracted with dichloromethane (3 x 100ml). The combined organic phases were dried (K2CO3) and concentrated and the residue triturated with hexanes to leave the product as a white solid, m.p. = 139-142°C.
b ) cis-3-( t-Butyldime thyl s ilyl o xy )- 6-keto - 1 -( 4- methoxybenzyl)-2-phenyl piperdine The product of part a) (2g) was dissolved in N,N-dimethylformamide (l5ml) with stirring and sodium hydride (80% in oil; 0.236g) was added. After 0.5h 4-methoxybenzylchloride (1.1ml) was added and the mixture stirred at 23°C for 16h, then diluted with water (150ml) and extracted with ethyl acetate (3 x 80ml). The combined organic phases were washed with brine (1 x 50ml) then dried (MgSO4) and concentrated to leave an oil. Purification on silica gel eluting with hexanes/ethyl acetate (4: 1 then 1:1 then ethyl acetate) provided the product as an oil. 1H NMR (250MHz, CDCl3)δ 7.36 (3H, m), 7.18 (2H, m), 7.04 (2H, d, J = 8.4Hz),
6.84 (2H, d, J = 8.4Hz),5 .52 (1H, d, J = 14Hz), 4.31 (1H, d, J = 4.2Hz), 4.02 (1H, m), 3.82 (3H, s), 3.32 (1H, d, J = 14Hz), 2.82 (1H, ddd, J = 5.5, 10.7, 18.2Hz), 2.64 (1H, m), 1.75 (2H, m), 0.78 (9H, s), -0.12 (3H, s), -0.28 (3H, s).
c ) cis-3-Hydroxy-6-keto- 1- ( 4- methoxybenzyl )- 2- phenylpiperdine The product of part b) ( 1.6g) was dissolved in tetrahydrofuran ( 10ml) and tetrabutylammonium fluoride ( 1M in tetrahydrofuran, 4.5ml) was added. After 3h saturated aqueous sodium hydrogen carbonate ( 10ml) was added and the mixture was extracted with ethyl acetate (3 x l5ml). The combined organic extracts were washed with brine (1 x 10ml) then dried (MgSO4 ) and concentrated to leave an oil. Purification on silica gel (hexanes/ethyl acetate 1:1 then ethyl acetate then methanol/ethyl acetate 1:9) provided the product as a white solid. 1H NMR (360MHz, CDCl3) 5 7.39 (3H, m), 7.21 (2H, dd, J = 1.8, 8.0Hz), 7.05 (2H, d, J = 8.6Hz), 6.83 (2H, d, J = 8.6Hz), 5.50 (1H, d, J = 14.5Hz), 4.48 (d, J = 5.3Hz), 4.04 (1H, m), 3.79 (3H, s), 3.29 (1H, d, J = 14.5Hz), 2.78 (1H, ddd, J = 5.5, 10.7, 18.2Hz), 2.60 (1H, m), 1.60 (2H, m); m/z (CI+) 312 (MH). d) cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-6-keto- 1-(4-methoxybenzyl)-2-phenyl piperidine The product of part c) (0.43g) was alkylated with 3,5-bis(trifluoromethyl)benzyl bromide (0.38ml) in an analogous manner to that described in Example 2d, to give the title compound as an oil. Analysis:
Found: C, 62.58; H, 4.86; N, 2.74. C28H25NO3F6 requires C, 62.57; H, 4.69; N, 2.61%; m/z (CI+) 538 (MH).
E X A M P L E 2 8 : c i s - 3 - ( ( 3 5 - Bis(trifluoromethyl)phenyl)methyloxy)-6-keto-2-phenyl piperidine
cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-6-keto-1- (4-methoxybenzyl)-2-phenyl piperidine (0.17g, Example 27) was dissolved in acetonitrile (3ml) and water (1ml) then cooled to 0°C and cerium ammonium nitrate ( 173mg) was added. The mixture was stirred at 23°C for 18h, then poured into water ( 10ml) and extracted with ethyl acetate ( 3 x 15ml ). The combined organic extracts were washed with brine (1 x 10ml) then dried (MgSO4) and concentrated to leave a pale yellow oil. Purification on silica gel (hexanes/ethyl acetate 1:1 then ethyl acetate then methanol/ethyl acetate 1:9) provided cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-6-keto-2-phenyl piperidine as an oil. 1H NMR (360MHz, CDCl3) 57.72 (1H, s), 7.44 (2H, s), 7.37 (5H, m), 5.86 (1H, s), 4.75 (1H, d, J = 3.2Hz), 4.52 (1H, d, J = 12.5Hz), 4.14 (1H, d, J = 12.5Hz), 3.98 (1H, m), 2.65 (1H, ddd, J = 6.4, 12.2, 18.2Hz), 2.48 (1H, m), 2.30 (1H, m), 2.06 (1H,m). m/z (CI+) 418 (MH).
E X A M P L E 2 9 : c i s - 3 - ( ( 3 , 5 -
Bis(trifluoromethyl)phenyl)methyloxy)-1-(2-carbomethoxy)ethyl- 2-phenylpiperidine
A s o l u t i o n o f c i s - 3 - ( ( 3 , 5 - bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine (1.3g, Example 4, free base) in methyl acrylate (30ml) was refluxed for 16h. The solvent was removed in vacuo and the residue purified on silica gel (ethyl acetate-petrol (b.p.60-80°C), 1:1) to provide the title compound as an oil. m/z (CI+) 490 (MH). 1H NMR
(360MHz, CDCI3)57.70 (1H, s), 7.47 (2H, s), 7.40-7.26 (5H, m), 4.44 (1H, d, J = 12.24Hz, OCHHPh), 4.00 (1H, J = 12.24Hz, OCHHPh), 3.57 (3H, s), 3.53 (1H, bs), 3.31 (1H, s), 3.17 (1H, bd), 2.96-2.89 (1H, m), 2.48-2.37 (3H, m), 2.27-2.0 (3H, m), 1.62-1.51 (3H, m). Found: C, 58.62; H, 5.20; N, 2.74. C24H25F6NO3 requires C, 58.90; H, 5.15; N, 2.86%. E X A M P L E 3 0 : c i s -3- ( ( 3 ,5 -
Bis(trifluoromethyl)phenyl)methyloxy)-1-(carboxamido)ethyl)-2- phenylpiperidine
A solution of the product of Example 29, (0.5g) in methanol (40ml) was saturated with ammonia at -30°C, sealed and stored at 25°C for 72h. The solution was evaporated to dryness and the residue chromatographed on silica gel eluting with ethyl acetate. The eluted product was concentrated and recrystallised from ethyl acetate to give the title compound, m.p. = 72-80°C; m/z (CI+) 475 (MH); Found: C, 58.51; H, 5.17; N, 5.63.
C23H24F6N2O2 requires C, 58.23; H, 5.10; N, 5.91%.
E X A M P L E 3 1 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyB)methyloxy)-1-(3- carbomethoxy)propyl-2-phenylpiperidine
A solution of the product of Example 4, (4g), methyl-4- bromobutyrate (2.4g) and potassium carbonate (3.8g) in dry dimethylformamide (20ml) was heated at 110°C for 16h. To the cooled solution was added ethyl acetate and water and the organic phase washed further with water and dried (MgSO4).
After the solvent had been removed in vacuo the residue was chromatographed on silica gel eluting with ethyl acetate/petrol (60-80°C) (1:9) to give the title compound, m.p. = 60-70°C. m/z (CI+) 504 (MH). Found: C, 59.65; H, 5.44; N, 2.81. C25H27F6NO3 requires C, 59.64; H, 5.41: N, 2.787%. E X A M P L E 3 2 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-(3-carboxamido)propyl- 2-phenylpiperidine
The title compound was prepared from the product of Example 31 using a procedure analogous to that described in
Example 30 and obtained as an oil, m/z (CI+) 489 (MH). Found:
C, 58.89; H, 5.64; N, 5.75. C24H26F6N2O2 requires C, 59.01; H,
5.37; N, 5.74%. EXAMPLE 33: (2S,3S)-1-t-Butoxycarbonyl-3-((3-methyl-5-
(trimethylsilyl)phenyl)methyloxy-2-phenylpiperidine
a) 3-Methyl-5-(trimethylsilyl)benzyl bromide
5-Bromo-m-xylene (12g) was added dropwise to a mixture of magnesium turnings (2.3 g) and iodine ( 1 crystal) in tetrahydrofuran (150ml) under a nitrogen atmosphere. The mixture was heated at reflux for 2h, then cooled. Freshly distilled trimethylsilyl chloride (16.4ml) was added to the mixture dropwise and the resulting mixture was stirred for 30 min. The solvent was removed in vacuo. The residue was washed with ammonium chloride solution, extracted with ether
(2 x 100ml) and dried (MgSO4). The ether was removed in vacuo to afford a brown oil. This oil (7.1g) was dissolved in carbon tetrachloride (40ml) under a nitrogen atmosphere. N- Bromosuccinimide (7.1g) and azobisisobutyronitrile (10mg) were added to the solution and the mixture was heated at 60°C for 2h.
The solvent was removed in vacuo and the residue was purified by chromatography on silica using hexane as eluant. This afforded 3-methyl-5-(trimethylsilyl)benzyl bromide as a brown oil. 1H NMR (360MHz, CDCl3)δ 0.26 (9H, s, Si(CH3)3), 2.35 (3H, s, CH3), 4.47 (2H, s, CH2Br), 7.20 (1H, s, ArH), 7.24 (1H, s, ArH), 7.30 (1H, s, ArH).
b) (+)-cis-3-Hydroxy-2-phenylpiperidine (Example 5c) was treated analogously to that described in Example 2c and then alkylated as described in Example 2d using 3-methyl-5- ( trimethylsilyl)benzyl bromide to give the title compound as a colourless oil. 1H NMR (360MHz, CDCI3 )δ 0.24 (9H, s, SICCH3)3), 1.46 (9H, s, NCOOC(CH3)3 ), 1.54-1.74 (2H, m, CH2), 1.85-2.00 (2H, m, CH2), 2.34 (3H, s, ArCH3), 2.65-2.76
(1H, m, NCHH), 3.77-3.87 (1H, m, NCHH), 3.88-3.96 (1H, bd, CHO), 4.56 ( 1H, d, J = 11.5Hz, OCHHAr), 4.67 (1H, d, J = 11.5Hz, OCHHAr), 5.73 (1H, bs, NHPh), 7.10 (1H, s, ArH), 7.22- 7.37 (5H, m, ArH), 7.60-7.62 (2H, 2s, Ar-H); MS (CI+) 454 (MH, 75%); Found: C, 71.75; H, 8.62; N, 3.25. C27H39NO3Si requires
C, 71.48; H, 8.66; N, 3.09.
EXAMPLE 34: cis-2-Phenyl-3-(phenylmethyloxy)piperidine oxalate salt
cis-1-t-Butyloxycarbonyl-3-hydroxy-2-phenylpiperidine
(Example 2c, 1g) was dissolved in dry dimethylformamide ( 10ml). Sodium hydride ( 163mg, 80% dispersion in oil) was added and the mixture was stirred for 30 minutes at room temperature. Benzyl bromide (923mg) was added and the mixture was stirred for 3h. Excess sodium hydride was destroyed (ammonium chloride), the mixture was diluted with water and extracted with ethyl acetate ( 2 x 30ml). The organic washings were washed with brine, dried (MgSO4) and evaporated. The crude residue was purified by chromatography on silica using petrol/ether (70:30) as eluant. The product was dissolved in ether and the solution cooled to 0°C. Anhydrous hydrogen chloride was bubbled through the solution for 30 min.
The ether was then evaporated and the crude product was dispersed between ethyl acetate and aqueous potassium carbonate. The organic extract was dried (MgSO4) and evaporated and the crude oil was purified by chromatography on silica using 7% methanol in dichloromethane as eluant. The product was dissolved in ethereal oxalic acid and recrystallised from ethyl acetate-ether, m.p. 150-151°C. 1H NMR (360MHz, CDCl3, free base) 5 1.58-1.72 (2H,.m, NCH2CH2CH2), 2.04-2.17 (2H,m, NCH2CH2), 2.94-3.02 (1H, m, CHHN), 3.36-3.39 (1H, m, -CHHN), 3.72 (1H, s, NCHCHO), 4.11 (1H, s, NCHCHO), 4.19
( 1H, d, J = 12.0Hz, OCHHPh), 4.35 ( 1H , d, J = 12.0Hz, OCHHPh), 7.00-7.03 (2H, m, ArH), 7.18-7.21 (3H, m, ArH), 7.31- 7.35 (3H, m, ArH), 7.39-7.41 (2H, m, ArH), 7.67 (1H, s, NH); MS (FAB) m/z 267 (MH, 25%). Found: C, 66.86; H, 6.44; N, 3.97. Calcd. for C18H21NO.(COOH)2.0.25H2O requires C, 66.56; H,
6.28; N, 3.88%.
EXAMPLE 35: cis-3-((3,5-Di-t-butylphenyl)methyloxy)-2- phenylpiperidine oxalate salt
a) 3,5-Di-t-butylbenzyl bromide
3,5-Di-t-butyltoluene (5g), N-bromosuccinimide (4.79g) and azobisisobutyronitrile ( 20mg) were dissolved in carbon tetrachloride (30ml) and the solution was heated at reflux for 3h. When cool, a white solid was removed by filtration, and the filtrate was concentrated yielding a yellow oil, which was used without further purification. 1H NMR (360MHz, CDCI3) δ 1.30 (18H, s, CH3), 4.45 (2H, s, CH2), 7.2 (2H, d, J = 1.75Hz, ArH),
7.4 (1H, s, ArH).
b) cis-3-((3,5-Di-(t-butyl)phenyl)methyloxy)-2- phenylpiperidine oxalate salt
This was prepared from cis-1-t-butyloxycarbonyl-3-hydroxy- 2-phenylpiperidine (Example 2c) and 3,5-di-t- butylbenzylbromide following the procedure described in Example 2d, e. m.p. = 205-207°C. 1H NMR (360MHz, CDCI3 free base)δ 1.25 (18H, s, CH3), 1.33-1.64 (2H, m, CH2CH2), 1.92-2.04 (1H, m, CHH), 2.18-2.21 (1H, m, CHH), 2.81-2.89 (1H, m, CHHN), 3.28-3.31 (1H, m, CHHN), 3.72 (1H, s, CHO), 3.88
(1H, s, NCHPh), 4.20 (1H, d, J = 12.0Hz, OCHH), 4.34 (d, J = 12.0Hz, OCHH), 6.92 (2H, d, J = 1.8Hz, ArH), 7.13-7.38 (4H, m, ArH), 7.43-7.45 (2H, m, ArH); MS (CI+) m/z, 380 (MH.100%). Found: C, 71.37; H, 8.43; N, 3.07. C26H36NO.(COOH)2 requires C, 71.61; H, 8.37; N, 2.98%.
EXAMPLE 36: (2S,3S)-3-((3-Methyl-5-iodo)phenyl)methyloxy)-2- phenylpiperidine hydrochloride
(2S,3S)-1-t-Butoxycarbonyl-3-((3-methyl-5- (trimethylsilyl)phenyl)methyloxy)-2-phenylpiperidine (Example
33.462mg) was dissolved in dry methanol (5ml) and stirred under nitrogen. The solution was cooled to 0°C and silver trifluoroacetate (500mg) was added. After 5 minutes iodine (259mg) was added which resulted in precipitation of a yellow solid; this was allowed to stir overnight. Methanol was removed in vacuo affording a yellow solid which was suspended in ethyl acetate (10ml) and filtered through celite to remove inorganic matter. The ethyl acetate solution was washed with sodium sulphite (2 x5 ml), brine ( 1 x5 ml), dried (MgSO4) and concentrated in vacuo to afford a clear oil. This was purified on silica using 5 % ethyl acetate in hexane as eluant. After evaporation of the solvent, the product was then cooled in an ice bath while trifluoroacetic acid (5ml) was added dropwise; the resulting solution was stirred for 30 min. Excess trifluoroacetic acid was removed in vacuo and the residue was partitioned between dichloromethane and aqueous sodium hydroxide solution. The aqueous layer was washed with dichloromethane (2 x 30ml) and the combined organic layers were washed with brine, dried (MgSO4) and evaporated to afford a yellow oil. This was dissolved in methanolic hydrogen chloride and evaporated. The resulting solid was recrystallised from ethyl acetate- methanol, m.p. = 207-209°C. 1H NMR (360MHz, CDCl3, free base)δ 1.4-2.0 (4H, m, NCH2CH2CH2), 2.15 (3H, s, CH3), 2.18
( 1H, m, NH), 2.78-2.86 ( 1H , m, NCHH), 3.24-3.29 ( 1H, m, NCHH), 3.60 (1H, s, CHO), 3.79 (1H, s, NCHPh), 4.01 (1H, d, J = 9.5Hz, OCHHAr), 4.29 (1H, d, J = 9.5Hz, OCHHAr), 6.65 (1H, s, ArH), 7.12 (1H, s, ArH), 7.24-7.36 (6H, m, ArH); Found: C, 51.66; H, 5.27; N, 3.12. C19H22NOI.HCl requires C, 51.43; H,
5.22; N, 3.15%. EXAMPLE 37: cis-3-(3,5-Bis(trifluoromethyl)phenyl)methyloxy)- 1-carbomethoxyformyl-2-phenyl piperidine
cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-2-phenyl piperidine hydrochloride salt (0.5g, Example 4) was suspended in dichloromethane (3ml) and triethylamine (0.477ml) was added followed by methyl oxalyl chloride (0.115ml). The reaction mixture was stirred at 23°C for 4h, then poured into saturated aqueous sodium bicarbonate solution (5ml) and extracted with dichloromethane (3 x 20ml). The combined organic phases were dried (MgSO4) and concentrated to leave an oil. Purification on silica gel (hexanes/ethyl acetate 3:1) provided the title compound as an oil. m/z (CI+) 490 (MH).
EXAMPLE 38: cis-3-(3,5-Bis(trifluoromethyl)phenyl)methyloxy)- 1-carboxamidoformyl-2-phenyl piperidine
The title compound was prepared from cis-3-(3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-carbomethoxyformyl-2- phenylpiperidine (Example 37) by a procedure analogous to that described in Example 7, m.p. = 78-81°C. Analysis: Found: C, 55.05; H, 4.39; N, 5.95. C22H22N2O3F6.[0.5CH3OH] requires
C, 55.11; H, 4.52; N, 5.71%.
EXAMPLE 39: cis-N-(1-Acetamidooxime)-3-(3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine The compound of Example 4 (800mg), hydroxylamine hydrochloride (188mg) and potassium carbonate (500mg) were suspended in ethanol ( 10ml) and the contents were heated at reflux for 5h. The mixture was cooled and evaporated and the residue was partitioned between dichloromethane and brine.
The organic layer was dried (MgSO4) and concentrated in vacuo. The resulting white solid was recrystallised from ethyl acetate and petrol, m.p.178-179°C. Η NMR (360MHz, CDCl3) δ 1.55 (2H, m,NCH2CH2CH2), 1.96-2.1 (3H, m, NCHHCH2CH2), 2.35 (1H, d, J = 14.0Hz, NCHH), 3.1 (1H, d, J = 14.0Hz,
NCHHCH2CH2), 3.32 (1H, d, J = 14.0Hz, NCHH), 3.34 (1H, s, CHO), 3.55 (1H, s, CHN), 4.02 (1H, d, J = 12.0Hz, OCHH), 4.45 (1H, d, J = 12.0Hz, OCHH), 5.07 (2H, s, NH2), 7.2-7.3 (4H, m, ArH+NOH), 7.55-7.4 (2H, d, J = 6.0Hz, ArH), 7.5 (2H, s, ArH), 7.70 (1H, s, ArH). MS (CI+) m/z 476 (MH). Found: C,55.4; H,
4.92; N, 8.94. Calcd. for C22H23N3O2F6: C, 56.58; H, 4.88; N, 8.84%.
E X A M P L E 4 0 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-cyanomethyl-2- phenylpiperidinium hydrochloride
The compound of Example 4 (5g), potassium carbonate (1.7g) and bromoacetonitrile (0.87ml) were suspended in dimethylformamide (15mi) and the mixture was stirred under nitrogen at 60°C for 3h. The mixture was cooled, diluted with water (200ml) and extracted with ethyl acetate (2 x 50ml). The organic extracts were washed with brine, dried (MgSO4) and evaporated, affording a brown oil. This was purified on silica gel using ethyl acetate in petrol (10%) as eluant. This afforded the product as a colourless oil. The hydrochloride salt was prepared by dissolution in ethereal hydrogen chloride and the salt was recrystallised from diethyl ether-hexane, m.p.133-134°C. 1H NMR (360MHz, CDCl3) δ 1.75 (2H, m, CHH), 1.90 (2H, m,
CHH), 2.31 (1H, mc, CHH), 2.71 (1H, m, CHH), 3.19 (1H, m, CHHN), 3.72 (1H, m, CHHN), 3.81 (1H, d, J = 17.5Hz, NCHHCN), 3.86 (1H, s, CHO), 4.02 (1H, d, J = 17.5Hz, NCHHCN), 4.09 (1H, s, CHPh), 4.35 (1H, d, J = 13.0Hz, OCHH), 4.73 (1H, d, J = 13.0Hz, OCHH), 7.4 (3H, m, ArH), 7.69-7.73
(5H, m, ArH); MS (CI+) m/z 443 (MH, 30%). Found: C, 54.87; H, 4.30; N, 5.66. Calcd. for C22H18F6N2O.HCl: C, 55.18; H, 4.42; N, 5.85%. E X A M P L E 4 1 : ( + ) - c i s - 3 - ( ( 3 , 5 -
Bis(trifluoromethyl)phenyl)methyloxy)-1-carboxymethyl-2- phenyl piperidine
The methyl ester (1.8g; Example 8) was dissolved in tetrahydrofuran (25ml) and a solution of potassium hydroxide (0.6g) in water (25ml) was added. The reaction mixture was heated at reflux for 18h, then the organic layer was removed in υacuo and the aqueous layer removed by freeze-drying. The residue was dissolved in the minimum volume of water and the pH adjusted to 7.0 by the addition of 2M hydrochloric acid. The precipitated solid was isolated by filtration and washed with water and then recrystallised from ethanol, m.p. = 60-63°C. Found: C, 53.11; H, 4.54; N, 3.05. Calcd. for C22H21F6NO3.HClC, 53.08: H, 4.45; N, 2.81%. m/z (CI+) 462 (MH). E X A M P L E 4 2 : c i s - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-((3,5- bis(trifluoromethyl)phenyl)methyl-2-phenylpiperidine
The title compound was prepared from cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine (Example 4) and 3,5-bis-trifluoromethyl benzyl bromide in an analogous manner to that described in Example 17. Found: C, 63.91; H, 3.62; N, 2.08. Calcd. for C29H23F12NO.0.3H2O C, 53.74; H, 3.89; N, 2.16%.
EXAMPLE 43: cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy- 1-(N,N-diethylcarboxamido)methyl-2-phenyl piperidinium hydrochloride
(+)-cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy)-1- carboxymethyl-2-phenyl piperidine (1g, Example 41), 1- hydroxybenzotriazole hydrate (1.2g), 1-(3-dimethylaminopropyl)- 3-ethyl-carbodiimide hydrochloride (1.66g), triethylamine (1.2ml) and diethylamine (0.55ml) were added together and the reaction was left stirring overnight at room temperature. The solvent was removed in vacuo and the residual yellow oil dispersed between water and ethyl acetate. The organic layer was washed with 1M citric acid, water, sodium hydrogen carbonate, brine, dried (MgSO4) and concentrated in vacuo to afford a yellow oil. This was purified on silica gel eluted with 50% ethyl acetate in petrol. The product was purified further by medium pressure chromatography eluting with 75% ethyl acetate in petrol to afford an oil. The hydrochloride salt was prepared (HCl, methanol) and crystallised from ethyl acetatehexane, m.p. = 135-137°C. Found: C, 55.66; H, 5.85; N, 4.90. C26H30N2O 2F6 squires C, 56.02; H, 5.70; N, 5.03%.
EXAMPLE 44: cis-3-((3-methyl-5-trimethylsilyl)benzyloxy)-2- phenyl piperidine
The Boc-protected ether (0.087g, Example 33) was dissolved in anhydrous dichloromethane (5ml) and stirred under nitrogen. t-Butyldimethylsilyl trifluoromethane sulfonate (0.044ml) was added and the reaction left overnight. The reaction mixture was washed with water, the organic layer was dried (MgSO4) and concentrated in vacuo to give a clear oil. Purification was carried out on silica gel eluting with dichloromethane then 3% methanol in dichloromethane to afford a clear oil. 1H NMR (360MHz, CDCl3 free base) 5 1.95 (9H, s, Si(CH3)3), 1.48-1.61 (2H, m, CH2), 1.92-2.18 (2H, m, CH2), 2.23 (3H, s, ArCH3), 2.78- 2.86 (1H, m, NCHH), 3.20-3.27 ( 1H, m, NCHH), 3.67 (1H, s, CHO), 3.95 ( 1H , s, NCHPh), 4.18-4.21 ( 1H, d, J = 12Hz, OCHHAr), 4.35-4.39 (1H, d, J = 12Hz, OCHHAr), 6.79 (H, s, ArH), 6.98 (H, s, ArH), 7.16 (H, s, ArH), 7.30-7.38 (5H, m, ArH). MS (CI+) m/z 354 (MH, 100%). EXAMPLE 45: cis-3-((2-Methoxy-5-nitrophenyl)methyloxy)-2- phenylpiperidine hydrochloride salt The Boc-protected alcohol (4.17g, Example 2c) was dissolved in N,N-dimethylformamide (15ml) under nitrogen, sodium hydride (0.03g) was added carefully and the mixture stirred for
0.5h. 2-Methoxy-5-nitro benzyl bromide (4.45g) was added and the solution changed colour from black to brown. After 3h the reaction was quenched with ammonium chloride. The product was extracted using ethyl acetate, dried and concentrated to afford a brown oil. This was purified on silica gel eluting with 5% ethyl acetate in hexane to provide an oil. This oil was dissolved in ether and then saturated with hydrogen chloride.
The precipitated solid was isolated by filtration and recrystallised from ethyl acetate-methanol, m.p. = 246-248°C. 1H NMR (360MHz, CDCl3 free base) 5 1.50-1.69 (1H, m, CHH), 1.64-1.75 (1H, m, CHH), 1.87-2.01 (1H, m, CHH), 2.22-2.32 (1H, m, CHH), 2.80-2.92 (1H, m, NCHH), 3.27-3.35 (1H, m, NCHH),
3.69 (1H, bs, CHO), 3.80 (3H, s, OCH3), 3.86 (1H, bs, NCHPh), 4.09-4.13 (1H, d, J = 13Hz, OCHHPh), 4.50-4.54 (1H, d, J = 13Hz, OCHHPh), 6.76-6.78 (1H, d, J = 9Hz. ArH), 7.20-7.40 (5H, m, ArH), 8.00-8.11 (2H, m, ArH). MS (CI+) m/z 343 (MH, 45%). Found: C, 60.52; H,5 .96; N, 7.45. C19H22N2O4.HCl requires C,
60.24; H, 6.12; N, 7.39%.
EXAMPLE 46: cis-3-((2-Methoxy-5-aminophenyl)methyloxy)-2- phenylpiperidine hydrochloride
The 5-nitro compound (0.324g, Example 45) was dissolved in methanol (20ml) with 1ml of 2N HCl. A spatula of wetted Pd/C was added and the reaction placed under an atmosphere of hydrogen for 1h at 23°C. The solvent was removed in vacuo and the residue basifϊed (2M NaOH) and extracted with ethyl acetate. The combined organic extracts were dried (MgSO4) and concentrated to leave a brown oil. Purification by column chromatography eluting with 8% methanol in dichloromethane provided an oil. The hydrochloride salt was prepared and recrystallised from ethyl acetate-methanol, m.p. = 241-243°C. 1H NMR (360MHz, CDCl3 free base)δ 1.25-1.66 (2H, m, CH2), 1.93-2.07 (1H, m, CHH), 2.23-2.31 (1H, m, CHH), 2.82-2.91 (1H, m, NCHH), 3.1-3.5 (3H, m, NH2 + NCHH), 3.64 (3H, s, OCH3),
3.70 (1H, bs, CHO), 3.89 (1H, bs, NCHPh), 4.22-4.25 (1H, d, J = 14Hz), 4.46-4.50 (1H, d, J = 14Hz, OCHHAr), 6.29 (1H, bs, ArH), 6.44-6.49 (1H, m, ArH), 6.55-6.57 (1H, d, J = 9Hz, ArH), 7.25- 7.38 (3H, m, ArH), 7.42-7.48 (2H, m, ArH).
EXAMPLE 47: cis-3-((3,5-Dichlorophenyl)methyloxy)-2- phenylpiperidine hydrochloride salt
T h e ti tl e c o mp o u n d w a s p r e p a r e d fr o m 1 - t - butyloxycarbonyl-3-hydroxy-2-phenylpiperidine (Example 2c) and 3,5-dichlorobenzylbromide in an analogous manner to that described in Example 2d, e , m.p. = 243-245°C. 1H NMR (360MHz, CDCI3) 51.49-1.63 ( 1H, m, CHH), 1.60-1.70 (1H, m, CHH), 1.82-1.95 (1H, m, CHH), 2.14-2.18 (1H, m, CHH), 2.79- 2.87 ( 1H, m, NCHH), 3.27-3.31 (1H, m, NCHH), 3.60 ( 1H, s, OCHCHN), 3.82 (1H, s, OCHCHN), 4.02-4.05 ( 1H, d, J = 13Hz,
OCHH), 4.31-4.35 ( 1H, d, J = 13Hz, OCHH), 6.80 (2H, s, ArH), 7.15 (1H, s, ArH), 7.25-7.36 (5H, m, ArH). Found: C, 58.24; H, 5.38; N, 3.91. Calcd. for C18H19NOCl2.HCl C, 58.01; H, 5.41; N, 3.76%. EXAMPLE 48: 3-((3,5-Bis(trifluoromethyl)ρhenyl)methyloxy)-3- methyl-2-phenylpiperidine oxalate salt
a) Oxalyl chloride (1ml) was added dropwise to a solution of methyl sulphoxide (0.82ml) in anhydrous dichloromethane (4ml) at -78°C under a nitrogen atmosphere. A solution of 1-t- butoxycarbonyl-3-hydroxy-2-phenyl piperidine (1.6g, Example
2c) in anhydrous dichloromethane ( 10ml) was added, and the reaction stirred for 1.75h before triethylamine (4ml) was added and the reaction allowed to warm to room temperature. The reaction was partitioned between ethyl acetate and water, the organic phase washed with brine, dried and evaporated in vacuo to provide 1-t-butoxycarbonyl-2-phenylpiperidin-3-one as an oil. b) A solution of 1-t-butoxycarbonyl-2-phenyl-piperidin-3-one (0.57g, Example 48a) in 5 ml anhydrous tetrahydrofuran at -78°C was treated with methyl magnesium bromide ( 1.6ml of 1.5M solution in toluene-THF). The reaction was partitioned between saturated ammonium chloride-diethyl ether, the organic phase dried and evaporated in vacuo. The residue was chromatographed using 20% ethyl acetate in hexane as eluant to give 1-t-butoxy carbonyl, 3-methyl-2-phenyl piperidin-3-ol as a crystalline solid, m.p. = 95-97°C. c) 1-t-Butoxycarbonyl-3-methyl-2-phenylpiperidin-3-ol
(Example 48b) was alkylated with 3, 5 - bis(trifluoromethyl)benzylbromide in a manner analogous to that described in Example 2d and then deprotected as described in Example 2e and the oxalate salt prepared and recrystallised from diethyl ether, m.p. = 230-232°C. 1H NMR (360MHz, d6-
DMSO) δ 1.05 (3H, s), 1.7-2.0 (3H, m), 2.3-2.4 (1H, m), 3.0-3.2
(1H, m), 3.3-3.4 (1H, m), 4.5 (1H, s), 4.6-4.8 (2H, m), 7.4-7.5 (3H, m), 7.5-7.6 (2H, m), 8.00 (1H, s), 8.1 (2H, s): Found: C, 53.04; H, 4.53; N, 2.64: C21H21NOF6.1.3C2H2O4 requires C, 53.04; H,
4.45; N, 2.64.
EXAMPLE 49: cis-3-((3,5-Bis(trifluoromethyl)ρhenyl)methyloxy- 1-(N-benzylcarboxamido)methyl-2-phenyl piperidinium hydrochloride
The title compound was prepared from (+)-cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-carboxymethyl-2- phenyl piperidine (Example 41) and benzylamine in an analogous manner to that described in Example 43, m.p. = 184- 186°C. Found: C, 59.63; H, 5.06; N, 4.67. C29H28N2F6.HCl requires C, 59.34; H, 4.98; N, 4.77%.
EXAMPLE 50: cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy- 1-(N-methylcarboxamido.methyl-2-phenyl piperidine
The title compound was prepared from cis-3-((3,5- bis(trifluoromethyl)phenyl)methyloxy)-1-(carbomethoxy)methyl- 2-phenyl piperidine (Example 6) and methylamine in an analogous manner to that described in Example 7. The hydrochloride salt was recrystallised from diethyl ether- hexanes, m.p. = 140-145°C. Found: C, 51.41; H, 5.17; N, 5.24. Calcd. for C23H24N2O2F6.1.5H2O C, 51.36; H, 5.25; N, 5.21%.
EXAMPLE 51: cis-3-((3,5-Dimethylphenyl)methyloxy)-1-methyl- 2-phenyl azetidine oxalate salt
a) To a suspension of sodium hydride ( 2.4g) in N,N- dimethylformamide (50ml) at 0°C was added a mixture of methyl glycolate (5g) and 3,5-dimethyl benzyl bromide dig. dropwise. The reaction was then quenched after 5 hours with iso-propanol/methanol solution. The reaction mixture was poured onto iced water and extracted with ether. The organic phase was dried (MgSO4), filtered and evaporated. The crude material was chromatographed on flash silica and eiuted with e thyl acetate : petrol ( 1 : 9 ) to affo rd me thyl - O -( 3 , 5 - dimethylbenzyl)glycolate as a solid.
b) To a solution of methyl O-(3,5-dimethylbenzyl)giycolate (7.47g) in methanol (100ml) aqueous sodium hydroxide (18ml) was added via pipette. Water was added dropwise until formation of a precipitate. The solvent was removed in vacuo, and the aqueous layer acidified using 2N HCl, then extracted with ethyl acetate. The organic phase was dried (MgSO4), filtered and evaporated to afford 3,5-dimethyl benzyl glycolic acid. 1H NMR (360MHz, CDCI3) δ 9.5 ( 1H, s, broad), 6.97 (1H. s), 6.95 (1H, s), 4.57 (2H, s), 4.12 (2H, s), 2.31 (6H, s).
c) 3,5-Dimethyl benzyl glycolic acid (5.59g) was cooled to 0°C. Thionyl chgloride (5ml) was added and the stirred solution was refluxed for 2h. The solvent was removed in vacuo to afford 3,5-dimethyl benzyl glycolic acid chloride as an oil.
d) To a solution of triethylamine (5.89g) in dichloromethane (50ml), N-benzylidenemethyl amine (3.09g) was added via syringe. The solution was cooled to 0°C and 3,5-dimethyl benzyl glycolic acid chloride (3.31g) in dichloromethane was added dropwise. After the solution had been stirred for 1h 5N HCl was added. The organic layer was washed with brine, dried, filtered and evaporated. The crude material was chromatographed on flash silica and eluted with ethyl acetate:petrol, 1:1 to afford 3; ((3,5-dimethylphenyl)methyloxy)-1-methyl-4-phenyl azetidin-2- one. 1H NMR (360MHz, CDCl3)δ 7.41 (3H, m), 7.33 (2H, m),
6.84 (1H, s), 6.48 (1H, s), 4.89 (1H, d, J = 4Hz), 4.67 (1H, d, J = 4Hz), 4.22 (1H, d, J = 11Hz), 4.08 (1H, d, J = 11Hz), 2.79 (1H, s), 2.20 (1H, s).
e ) To a solution o f aluminium chloride ( 0.29g) in tetrahydrofuran (10ml), lithium aluminium hydride (2.2ml) was carefully added dropwise. After the reaction mixture had been stirred for lh, a solution of 3-((3,5-dimethylphenyl)methyloxy)-1- methyl-4-phenyl azetidin-2-one (0.66g) in tetrahydrofuran (5ml) was added via syringe. After a further hour water ( 1ml) was carefully added dropwise followed by dropwise addition of 2N sodium hydroxide ( 1ml). Dichloromethane (75ml) was added followed by magnesium sulphate. After stirring for 30 minutes the solution was filtered. The organic phase was dried (MgSO4), filtered and evaporated. The crude material was chromatographed on flash silica and eluted with ethyl acetate.petrol 1:1. The resulting compound was dissolved in ether and an ethereal solution of oxalic acid was added dropwise to give the title compound as a white solid, m.p. = 147-149°C.1H NMR (360MHz, DMSO) δ 7.57 (2H, m), 7.43 (3H, m), 6.86 (1H, s), 6.62 (1H, s), 5.02 (m), 4.55 (m), 4.17 (1H, d, J = 11Hz), 3.94 (1H, d, J = 11Hz), 3.83 (1H, s), 2.61 (1H, s), 2.19 (1H, s); m/z
(CI+) 282 (MH). Found: C, 67.75; H, 7.00; N, 3.78. Calcd for C19H23O1N1- [COOH]2: C, 67.91; H, 6.78; N, 3.77%.
EXAMPLE 52: cis-3-((3-Bromophenyl)methyloxy)-2- phenylpiperidine hydrochloride salt
The title compound was prepared from 1-t- butyloxycarbonyl-3-hydroxy-2-phenyl piperidine (Example 2c) and 3-bromobenzyl bromide in an analogous manner to that described in Example 2d, e, m.p.215-220°C; m/z (CI+) 346 (MH); Analysis: Found: C, 56.90; H, 5.56; N, 3.68. Calcd for
C18H20BrNO.HCl; C, 56.49; H, 5.53; N, 3.66%.
EXAMPLE 53: cis-3((3-Cyanophenyl)methyloxy)-2- phenylpiperidine hydrochloride salt
The title compound was prepared from 1-t- butyloxycarbonyl-3-hydroxy-2-phenyl piperidine (Example 2c) and α-bromo-m-tolunitrile in an analogous manner to that described in Example 2d, e, m.p. 168-178°C; m/z (CI+) 293 (MH).
EXAMPLE 54 : cis- 3 -( ( 3 - C arb oxyphenyl )methyloxy- 2- phenylpiperidine
cis-1-t-Butyloxycarbonyl-3-((3-cyanophenyl)methyloxy)-2- phenylpiperidine (prepared as an intermediate, Example 53, 3g, 7.3mmol) was refluxed in concentrated hydrochloric acid- methanol (1:1) for 16h. The mixture was cooled and adjusted to pH 7 with sodium hydroxide, and the product extracted into ethyl acetate. The organic phase was washed (H2O), dried
(MgSO4) and the solvent removed in vacuo. The residue was triturated with ether to give a white solid, m/z (CI+) 326 (MH).
EXAMPLE 65: cis-3-((3,5-Bis(trifluoromethyl)phenyl)methyloxy- 6-hydroxymethyl-2-phenyl piperidine
Mercuric acetate (4.92g) was added to a solution of N-Boc-2- ( (3 ,5-bis(trifluoromethyl)phenyl)methyloxy)-1-phenyl-hex-5-enyl- 1-amine (4g, Example 20) in tetrahydrofuran (80ml) at 50°C and the mixture stirred at this temperature for 16h. The solvent was removed in vacuo and the residue dissolved in chloroform and mixed thoroughly with saturated potassium chloride solution. The layers were separated, and the aqueous phase extracted with chloroform ( 1 x5 0ml). The combined organic phases were dried (MgSO4) and concentrated to leave a palevellow solid. This material was dissolved in N,N-dimethylformamide
(28ml) and added dropwise during 16 min to a saturated solution of oxygen in N,N-dimethylformamide (24ml) with continuous infusion of oxygen. The reaction mixture was stirred at 23°C for lh, then diluted with diethyl ether (300ml) and filtered through a pad of Celite. The filtrate was diluted with water (300ml) and extracted with ethyl acetate (3 x 150ml). The combined organic phases were washed with water (1 x 150ml) and brine (1 x 150ml) then dried (MgSO4) and concentrated to leave an oil. Purification on silica gel eluting with hexanesethyl acetate (9:1 then 4:1 then 1:1) provided a clear oil.
This material was dissolved in trifluoroacetic acid (10ml) and allowed to stand at 23°C for 10 min. The trifluoroacetic acid was removed in vacuo and the residue dissolved in dichloromethane (30ml) and washed with 2M sodium hydroxide solution (2 x 10ml), brine (1 x 10ml) then dried (MgSO4) and concentrated to leave an oil. Purification on silica gel eluting with hexanes-ethyl acetate (1% triethylamine; 4:1 then 3:1 then 1:1) then ethyl acetate provided the title compound as an oil. m/z (CI+) 434 (MH).
E X A M P L E 5 6 : ( 2 S , 3 S ) - 3 - ( ( 3 , 5 -
Bis(trifluoromethyl)phenyl)methyloxy)-1-((N-t- butyl)carboxamidomethyl)-2-phenylpiperidinium hydrochloride The compound of Example 41 was reacted with t- butylamine according to the procedure described in Example 43 to afford the title compound, m.p.74-76°C. 1B. NMR (360MHz, DMSO-dg, free base)δ 1.22 (9H, s, C(CH3)3), 1.52-1.65 (2H, m, CH2), 1.87-1.91 (1H, m, CHH), 2.16-2.19 (1H, m, CHH), 2.32- 2.35 (1H, m, NCHH), 2.38 (1H, d, J = 16.0Hz, NCHHC=O), 2.75 (1H, d, J = 16.0Hz, NCHHC=O), 2.89-2.92 (1H, m, NCHH), 3.69 (1H, s, NCHCHO), 3.63 (1H, s, NCHHO), 4.10 (1H, d, J = 13.0Hz, OCHH), 4.68 (1H, d, J = 13.0Hz, OCHH), 7.24-7.28 (3H, m, ArH), 7.40-7.46 (2H, m, ArH), 7.82 (2H, s, ArH), 7.96 (1H, s, ArH); MS (CI+) m/z 516 ((MH), 100%).
E X A M P L E 5 7 : ( 2 S , 3 S ) - 3 - ( ( 3 , 5 - Bis(trifluoromethyl)phenyl)methyloxy)-1-((N- cyclopropyl)carboxamidomethyl)-2-phenylpiperidinium hydrochloride
The compound of Example 41 was reacted with cyclopropylamine according to the procedure described in Example 43 to afford the title compound. 1H NMR (360MHz, CDCl3)δ 0.49 (2H, m, CH2-cyclopropyl), 0.80 (2H, m, CH2- cyclopropyl), 1.50-1.68 (2H, m, CH2).2.04-2.27 (3H, m, CH2 + NCHH), 2.50 (1H, br d, NCHHC = 0), 2.70 (2H, m, CH- cyclopropyl), 3.00 (1H, m, NCHH), 3.14 (1H, br d, NCHHC=O), 3.43 (1H, brs, CHO), 3.68 (1H, brs, NCHPh), 4.03 (1H, d, J = 12.0Hz, OCHH), 4.48 (1H, d, J = 12.0Hz, OCHH), 7.26-7.30 (6H, m. ArH+NH), 7.56 (2H, s, ArH), 7.75 (1H, s, ArH). MS (CI+) m/z 501 (MH). The following examples illustrate pharmaceutical
compositions according to the invention.
EXAMPLE 58A Tablets containing 1-25mg of compound
Amount mg
Compound of formula (I) 1.0 2.0 25.0 Microcrystalline cellulose 20.0 20.0 20.0 Modified food corn starch 20.0 20.0 20.0 Lactose 58.5 57.5 34.5 Magnesium Stearate 0.5 0.5 0.5
EXAMPLE 58B Tablets containing 26-100mq of compound
Amount mg
Compound of formula (I) 26.0 50.0 100.0 Microcrystalline cellulose 80.0 80.0 80.0
Modified food corn starch 80.0 80.0 80.0
Lactose 213.5 189.5 139.5
Magnesium Stearate 0.5 0.5 0.5
The compound of formula (I), cellulose, lactose and a portion of the corn starch are mixed and granulated with
10% corn starch paste. The resulting granulation is sieved, dried and blended with the remainder of the corn starch and the magnesium stearate. The resulting granulation is then compressed into tablets containing 1.0mg, 2.0mg, 25.0mg, 26.0mg, 50.0mg and 100mg of the active compound per tablet.
EXAMPLE 59 Parenteral injection
Amount mg
Compound of formula (I) 1 to 100mg
Citric Acid Monohydrate 0.75mg
Sodium Phosphate 4.5mg
Sodium Chloride 9mg
Water for Injections to 1ml The sodium phosphate, citric acid monohydrate and sodium chloride are dissolved in a portion of the water. The compound of formula (I) is dissolved or suspended in the solution and made up to volume.
EXAMPLE 60 Topical formulation
Amount mg
Compound of formula (I) 1-10g
Emulsifying Wax 30g
Liquid paraffin 20g
White Soft Paraffin to 100g
The white soft paraffin is heated until molten. The liquid paraffin and emulsifying wax are incorporated and stirred until dissolved. The compound of formula (I) is added and stirring continued until dispersed. The mixture is then cooled until solid.
SUBSTANCE P ANTAGONISM ASSAY A. Receptor Expression in Monkey Kidney Cell Line (COS)
To express the cloned human neurokinin-1- receptor (NK1R) transiently in COS, the cDNA for the human NK1R was cloned into the expression vector pCDM9 which was derived from pCDM8 (INVITROGEN) by inserting the
ampicillin resistance gene (nucleotide 1973 to 2964 from BLUESCRIPT SK+ (trademark, STRATAGENE, La Jolla, CA, USA)) into the Sac II site. Transfection of 20 ug of the plasmid DNA into 10 million COS cells was achieved by electroporation in 800 μl of transfection buffer (135 mM NaCl, 1.2 mM CaCl2, 1.2 mM MgCl2, 2.4 mM K2HPO4, 0.6 mM
KH2PO4, 10 mM glucose, 10 mM N-2-hydroxyethyl-piperazine- N'-2-ethane sulphonic acid (HEPES) pH 7.4) at 260 V and 950 μF using the IBI GENEZAPPER (trademark IBI, New
Haven, CT, USA). The cells were incubated in 10% fetal calf serum, 2 mM glutamine, 100U/ml penicillinstreptomycin, and 90% DMEM media (GIBCO, Grand Island, NY, USA) in 5% CO2 at 37°C for three days before the binding assay.
B. Stable Expression in Chinese Hamster Ovarian Cell Line (CHO)
To establish a stable cell line expressing cloned human NKIR, the cDNA was subcloned into the vector pRcCMV (INVITROGEN). Transfection of 20 μg of the plasmid DNA into CHO cells was achieved by electroporation in 800 μl of transfection buffer supplemented with 0.625 mg/ml Herring sperm DNA at 300 V and 950 μF using the IBI
GENEZAPPER (IBI). The transfected cells were incubated in CHO media [10% fetal calf serum, 100 U/ml penicillinstreptomycin, 2 mM glutamine, 1/500 hypoxanthinethymidine (ATCC), 90% IMDM media (JRH BIOSCIENCES,
Lenexa, KS, USA), 0.7 mg/ml G418 (GIBCO)] in 5% CO2 at 37°C until colonies were visible. Each colony was separated and propagated. The cell clone with the highest number of human NKIR was selected for subsequent applications such as drug screening.
C. Assay Protocol using COS or CHO
The binding assay of human NKIR expressed in either
COS or CHO cells is based on the use of 125I-substance P (125I-SP, from DU PONT, Boston, MA) as a radioactively labeled ligand which competes with unlabeled substance P or any other ligand for binding to the human NKIR.
Monolayer cell cultures of COS or CHO were dissociated by the non-enzymatic solution (SPECIALTY MEDIA, Lavellette, NJ) and resuspended in appropriate volume of the binding buffer (50 mM Tris pH 7.5, 5 mM MnCl2, 150 mM NaCl, 0.04 mg/ml bacitracin, 0.004 mg/ml leupeptin, 0.2 mg/ml BSA, 0.01 mM phosphoramidon) such that 200 μl of the cell suspension would give rise to about 10,000 cpm of specific 125I-SP binding (approximately 50,000 to 200,000 cells). In the binding assay, 200 μl of cells were added to a tube containing 20 μl of 1.5 to 2.5 nM of 125I-SP and 20 μl of unlabeled substance P or any other test compound. The tubes were incubated at 4°C or at room temperature for 1 hour with gentle shaking. The bound radioactivity was separated from unbound radioactivity by GF/C filter (BRANDEL, Gaithersburg, MD) which was prewetted with 0.1% polyethylenimine. The filter was washed with 3 ml of wash buffer (50 mM Tris pH 7.5, 5 mM MnCl2, 150 mM NaCl) three times and its radioactivity was determined by gamma counter.
The activation of phospholiphase C by NKIR may also be measured in CHO cells expressing the human NKIR by determining the accumulation of inositol monophosphate which is a degradation product of IP3. CHO cells are seeded in 12-well plate at 250,000 cells per well. After incubating in CHO media for 4 days, cells are loaded with 5μCi of 3H-myoinositol in 1 ml of media per well by overnight incubation. The extracellular radioactivity is removed by washing with phosphate buffered saline. LiCl is added to the well at final concentration of 10 mM with or without the test compound, and incubation is continued at 37°C for 15 min. Substance P is added to the well at final concentration of 0.3nM to activate the human NKIR. After 30 min of incubation at 37°C, the medium is removed and 0.1 N HCl is added. Each well is sonicated at 4°C and extracted with CHCl3/methanol (1:1). The aqueous phase is applied to a 1 ml Dowex AG 1X8 ion exchange column. The column is washed with 0.1 N formic acid followed by 0.025 M ammonium formate-0.1 N formic acid. The inositol monophosphate is eluted with 0.2 M ammonium formate-0.1 N formic acid and quantitated by beta counter.
The data in Table 1 were obtained for compounds of formula (I):
Figure imgf000087_0001
Figure imgf000088_0001
Figure imgf000089_0001

Claims

1. A compound of formula (I), or a salt or prodrug thereof:
Figure imgf000090_0001
(l)
wherein
n is 1, 2 or 3 and any carbon atom of (CH2)n may be substituted by R4 and/or R5;
X represents O or S;
R1 represents phenyl optionally substituted by 1, 2 or 3 groups selected from C1-6 alkyl, C2-6 alkenyl,
C2-6alkynyl, halo, cyano, nitro, trifluoromethyl, trimethylsilyl, -ORa, SRa, SORa, SO2Ra, -NRaRb, -NRaCORb, -NRaCO2Rb, -CO2Ra or -CONRaRb;
R2 represents aryl selected from phenyl and
naphthyl; heteroaryl selected from indazolyl, thienyl, furyl, pyridyl, thiazolyl, tetrazolyl and quinolyl;
benzhydryl; or benzyl; wherein each aryl or heteroaryl moiety may be substituted by C1-6alkyl, C2-6 alkoxy, halo or trifluoromethyl;
R4 and R5 each independently represent H, halo,
CH2OR9, C2-6alkyl, oxo, CO2R10 or CONR10R11 ;
R8 represents H, COR9, CO2R10, COCONR10R11, COCO2R10 or C2-6alkyl optionally substituted by a group selected from (CO2R10, CONR10R11, hydroxy, cyano, COR9, NR10R11, C(NOH)NR10R11, CONHphenyl(C1-4alkyl), COCO2R10,
COCONR10R11 and phenyl optionally substituted by one or more substituents selected from C1-6alkyl, C1-6alkoxy, halo and trifluoromethyl);
Ra and Rb each independently represent H, C1-6alkyl, phenyl or trifluoromethyl;
R9 represents H, C1-6alkyl or phenyl; and
R10 and R11 each independently represent H or
C1-6alkyl.
2. A compound as claimed in claim 1 wherein n is 2 or 3; R4 and R5 each independently represent H, halo, C1-6alkyl, CO2R10 or CONR10R11; and R8 represents H, COR9 or C1-6alkyl optionally substituted by a group selected from (CO2R10, CONR10R11 and phenyl optionally substituted by C1-6alkyl, C1-6alkoxy, halo or trifluoromethyl).
3. A compound as claimed in claim 2 wherein R2 represents phenyl or benzhydryl wherein any of the phenyl rings of the phenyl or benzhydryl moieties may optionally be substituted by halo or trifluoromethyl; R4 and R5 each independently represent H, C1-6alkyl or CO2 (C1-6alkyl); and R8 represents H or C1-6alkyl.
4. A compound as claimed in claim 1 wherein R1 represents phenyl substituted by one or more substituents selected from C1-6alkyl, nitro, trifluoromethyl, COOH, trimethylsilyl, bromo, chloro, iodo, cyano, C1-6alkoxy and amino; R2 represents unsubstituted or substituted phenyl, thienyl, pyridyl or benzhydryl; R4 and R5 each independently represent H, C1-6alkyl, hydroxymethyl or oxo; and R8 represents H, COR9, CO2R10, COCONR10R11, COCO2R10, C1-6alkyl or C1-6alkyl substituted by CO2R10, CONR10R11 , cyano, C(NOH)NR10R11, CONHphenyl (C1-4alkyl), or optionally substituted phenyl.
5. A compound as claimed in any one of claims 1, 2 and 4 wherein R8 represents C1-6alkyl substituted by
CO2R10 or CONR10R11.
6. A compound as claimed in any preceding claim wherein n is 3.
7. A compound as claimed in any preceding claim wherein R2 is unsubstituted phenyl.
8. A compound as claimed in claim 1 selected from: cis-2-(diphenylmethyl)-3-(3,5-dimethylbenzyloxy)-1- methylpyrrolidine;
cis-3-((3,5-dimethylphenyl)methyloxy)-2-phenylpiperidine; cis-3-((3,5-dimethylphenyl)methyloxy)-1-methyl-2- phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2- phenylpiperidine;
(+)-cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- (carbomethoxy)methyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-
(carboxamido)methyl-2-phenylpiperidine;
(+)-cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-
(carbomethoxy)methyl-2-phenylpiperidine;
(+)-cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-
(carboxamido)methyl-2-phenylpiperidine;
(+)-cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- methyl-2-phenylpiperidine; (-)-cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2- phenylpiperidine;
trans-3-((3,5-dimethylphenyl)methyloxy)-2- phenylpiperidine;
trans-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-phenylpiperidine;
(2S,3S)-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-
1,1-dimethyl-2-phenylpiperidine;
(2S,3S)-1-acetyl-3-((3,5-bis(trifluoromethyl)phenyl) methyloxy)-2-phenylpiperidine;
(2S,3S)-1-formyl-3-((3,5-bis(trifluoromethyl)phenyl) methyloxy)-2-phenylpiperidine;
(2S,3S)-1-benzyl-3-((3,5-bis(trifluoromethyl)phenyl) methyloxy)-2-phenylpiperidine;
(2S,3S)-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-
(1-carbomethoxy)ethyl-2-phenylpiperidine;
(2S,3S)-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-
(1-carbσxamido)ethyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-6- methyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-(2- chlorophenyl)piperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-(3- chlorophenyl)piperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-(4- chlorophenyl)piperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-(4- methylphenyl)piperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2- thienylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2- pyridylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-6-keto-
1-(4-methoxybenzyl)-2-phenylpiperidine; cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-6-keto-
2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-(2- carbomethoxy)ethyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-
(carboxamido)ethyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-(3-carbomethoxy)propyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-(3- carboxamido)propyl-2-phenylpiperidine;
(2S,3S)-1-t-butoxycarbonyl-3-((3-methyl-5-
(trimethylsilyl)phenyl)methoxy-2-phenylpiperidine;
cis-2-phenyl-3-(phenylmethyloxy)piperidine;
cis-3-((3,5-di-t-butylphenyl)methyloxy)-2- phenylpiperidine;
(2S,3S)-3-(((3-methyl-5-iodo)phenyl)methyloxy)-2- phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-carbomethoxyformyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- carboxamidoformyl-2-phenylpiperidine;
cis-N-(1-acetamidooxime)3-((3,5-bis(trifluoromethyl) phenyl)methyloxy)-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- cyanomethyl-2-phenylpiperidine;
(+)-cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- caraboxymethyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- ((3,5-bis(trifluoromethyl)phenyl)methyl)-2- phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-(N,N-diethylcarboxamido)methyl-2-phenylpiperidine;
cis-3-((3-methyl-5-trimethylsilyl-benzyloxy)-2- phenylpiperidine; cis-3-((2-methoxy-5-nitrophenyl)methyloxy)-2- phenylpiperidine;
cis-3-((2-methoxy-5-aminophenyl)methyloxy)-2- phenylpiperidine;
cis-3-((3,5-dichlorophenyl)methyloxy)-2-phenylpiperidine; 3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-3-methyl-2- phenylpiperidine;
3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-2-methyl-2- phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-(N- benzylcarboxamido)methyl-2-phenylpiperidine;
cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1-(N- methylcarboxamido)methyl-2-phenylpiperidine;
cis-3-((3,5-dimethylphenyl)methyloxy)-1-methyl-2- phenylazetidine;
cis-3-((3-bromophenyl)methyloxy)-2-phenylpiperidine;
cis-3-((3-cyanophenyl)methyloxy)-2-phenylpiperidine;
cis-3-((3-carboxyphenyl)methyloxy)-2-phenylpiperidine; cis-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-6- hydroxymethyl-2-phenylpiperidine;
(2S,3S)-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- (N-t-butylcarboxamidomethyl)-2-phenylpiperidine;
(2S,3S)-3-((3,5-bis(trifluoromethyl)phenyl)methyloxy)-1- ((N-cyclopropyl)carboxamidomethyl)-2-phenylpiperidine; and salts and prodrugs thereof.
9. A compound as claimed in any preceding claim for use in therapy.
10. A pharmaceutical composition comprising a compound as claimed in any of claims 1 to 8 in
association with a pharmaceutically acceptable carrier.
11. A process for the preparation of a compound as claimed in claim 1, which process comprises reacting a compound of formula (III) with a compound of formula (IV):
Figure imgf000096_0001
(III) (IV) wherein R1, R2, R4, R5 and n are as defined for formula (I), R8 is as defined for formula (I) except that, when R8 is H it is replaced by a suitable protecting group, such as CO2 (C1-6alkyl); and one of R30 and R31 represents a leaving group and the other of R30 and R31 represents XH, where X is as defined for formula (I); in the presence of a base, followed by deprotection, if
required; and optionally converting the compound of formula (I) so prepared to another compound of formula (I), or a salt or prodrug thereof.
12. A method for the treatment or prevention of a physiological disorder associated with an excess of tachykinins, which method comprises administration to a patient in need thereof of a tachykinin-reducing amount of a compound according to claim 1.
13. A method according to claim 12 for the
treatment or prevention of pain or inflammation.
14. A method according to claim 12 for the
treatment or prevention of migraine.
15. A method according to claim 12 for the
treatment or prevention of postherpetic neuralgia.
16. A compound as claimed in any of claims 1 to 8 when prepared by the process of claim 11.
17. A process for preparing a composition as claimed in claim 10 which process comprises bringing a compound as claimed in any of claims 1 to 8 into
association with a pharmaceutically acceptable carrier or excipient.
18. A compound, composition or process as claimed in any one of the preceding claims, substantially as herein before described.
PCT/GB1992/001503 1991-08-20 1992-08-13 Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them Ceased WO1993004040A1 (en)

Priority Applications (6)

Application Number Priority Date Filing Date Title
EP92917251A EP0600952B1 (en) 1991-08-20 1992-08-13 Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them
DE69210029T DE69210029T2 (en) 1991-08-20 1992-08-13 AZACYCLIC COMPOUNDS, METHOD FOR THE PRODUCTION THEREOF AND PHARMACEUTICAL PREPARATIONS CONTAINING THEM
US08/196,269 US5459270A (en) 1991-08-20 1992-08-13 Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them
AT92917251T ATE136885T1 (en) 1991-08-20 1992-08-13 AZACYCLIC COMPOUNDS, METHOD FOR THE PRODUCTION THEREOF AND PHARMACEUTICAL PREPARATIONS CONTAINING THEM
AU24138/92A AU661711B2 (en) 1991-08-20 1992-08-13 Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them
JP5504179A JPH06510034A (en) 1991-08-20 1992-08-13 Azacyclic compounds, methods for their production, and pharmaceutical compositions containing them

Applications Claiming Priority (6)

Application Number Priority Date Filing Date Title
GB919117934A GB9117934D0 (en) 1991-08-20 1991-08-20 Therapeutic agents
GB9117934.1 1991-08-20
GB9125619.8 1991-12-02
GB919125619A GB9125619D0 (en) 1991-12-02 1991-12-02 Therapeutic agents
GB9204119.3 1992-02-26
GB929204119A GB9204119D0 (en) 1992-02-26 1992-02-26 Therapeutic agents

Publications (1)

Publication Number Publication Date
WO1993004040A1 true WO1993004040A1 (en) 1993-03-04

Family

ID=27265831

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/GB1992/001503 Ceased WO1993004040A1 (en) 1991-08-20 1992-08-13 Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them

Country Status (9)

Country Link
US (1) US5459270A (en)
EP (2) EP0528495A1 (en)
JP (1) JPH06510034A (en)
AT (1) ATE136885T1 (en)
AU (1) AU661711B2 (en)
CA (1) CA2112397A1 (en)
DE (1) DE69210029T2 (en)
IL (1) IL102833A0 (en)
WO (1) WO1993004040A1 (en)

Cited By (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
GB2268931A (en) * 1992-07-22 1994-01-26 Merck Sharp & Dohme Azabicyclic tachykinin-receptor antagonists
FR2766366A1 (en) * 1997-07-24 1999-01-29 Seppic Sa USE OF AT LEAST ONE LIPOAMINOACID AS AN ANTAGONIST OF THE SUBSTANCE P IN A COSMETIC FORMULATION FOR SOOTHING AND / OR PROTECTING ALL SKIN TYPES AND, IN PARTICULAR, SENSITIVE SKIN
EP0743939B1 (en) * 1994-02-11 2000-05-10 MERCK SHARP & DOHME LTD. Aralkoxy and aralkylthio substituted azacyclic compounds as tachykinin antagonists
US6203803B1 (en) 1994-12-14 2001-03-20 Societe L'oreal S.A. Use of a substance P antagonist in a cosmetic composition, and the composition thus obtained
US6235291B1 (en) 1994-05-05 2001-05-22 Societe L'oreal S.A. Use of a substance P antagonist in a cosmetic composition, and the composition thus obtained
WO2025008409A2 (en) 2023-07-03 2025-01-09 Preeti Jha Substituted 2-phenylpiperidine compounds for use in the diagnosis, treatment and/or prevention of cancer

Families Citing this family (91)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO1993021181A1 (en) * 1992-04-15 1993-10-28 Merck Sharp & Dohme Limited Azacyclic compounds
US5719147A (en) * 1992-06-29 1998-02-17 Merck & Co., Inc. Morpholine and thiomorpholine tachykinin receptor antagonists
CA2099233A1 (en) * 1992-06-29 1993-12-30 Conrad P. Dorn Morpholine and thiomorpholine tachykinin receptor antagonists
US5637699A (en) * 1992-06-29 1997-06-10 Merck & Co., Inc. Process for preparing morpholine tachykinin receptor antagonists
US6048859A (en) * 1992-06-29 2000-04-11 Merck & Co., Inc. Morpholine and thiomorpholine tachykinin receptor antagonists
US5561130A (en) * 1992-07-28 1996-10-01 Merck Sharp & Dohme Limited Azacyclic compounds
FR2700472B1 (en) 1993-01-19 1995-02-17 Rhone Poulenc Rorer Sa Synergizing association having an antagonistic effect on the NK1 and NK2 receptors.
AU679207B2 (en) * 1993-02-18 1997-06-26 Merck Sharp & Dohme Limited Azacyclic compounds, compositions containing them and their use as tachykinin antagonists
US5817679A (en) 1993-04-01 1998-10-06 University Of Virginia 7-Azabicyclo 2.2.1!-heptane and -heptene derivatives as cholinergic receptor ligands
US6060473A (en) * 1993-04-01 2000-05-09 Ucb S.A. - Dtb 7-azabicyclo[2.2.1]-heptane and -heptene derivatives as cholinergic receptor ligands
GB9315808D0 (en) * 1993-07-30 1993-09-15 Merck Sharp & Dohme Therapeutic agents
CN1137753A (en) * 1993-09-10 1996-12-11 赛托医学有限公司 Epibatidine and derivatives thereof as cholinergic receptor agonists and antagonists
WO1995011895A1 (en) * 1993-10-26 1995-05-04 Ciba-Geigy Ag N-benzoyl-4-oxy/thio-2-substituted piperidines as substance-p receptor antagonists
IL111960A (en) * 1993-12-17 1999-12-22 Merck & Co Inc Morpholines and thiomorpholines their preparation and pharmaceutical compositions containing them
WO1995018124A1 (en) * 1993-12-29 1995-07-06 Merck Sharp & Dohme Limited Substituted morpholine derivatives and their use as therapeutic agents
US5610165A (en) * 1994-02-17 1997-03-11 Merck & Co., Inc. N-acylpiperidine tachykinin antagonists
TW385308B (en) * 1994-03-04 2000-03-21 Merck & Co Inc Prodrugs of morpholine tachykinin receptor antagonists
US5863903A (en) * 1994-03-09 1999-01-26 Novo Nordisk A/S Use of hydroxy alkyl piperidine and pyrrolidine compounds to treat diabetes
US6117889A (en) * 1994-04-01 2000-09-12 University Of Virginia 7-Azabicyclo-[2.2.1]-heptane and -heptene derivatives as analgesics and anti-inflammatory agents
FR2719476B1 (en) * 1994-05-05 1997-05-23 Oreal Use of a substance P antagonist in a cosmetic composition and composition obtained.
EP0777659B1 (en) * 1994-08-15 2001-06-06 MERCK SHARP & DOHME LTD. Morpholine derivatives and their use as therapeutic agents
GB9417956D0 (en) * 1994-09-02 1994-10-26 Merck Sharp & Dohme Therapeutic agents
ES2172595T3 (en) * 1994-09-30 2002-10-01 Novartis Ag COMPOUNDS OF 1-ACIL-4-ALIFATILAMINOPIPERIDINA.
FR2728166A1 (en) 1994-12-19 1996-06-21 Oreal TOPICAL COMPOSITION CONTAINING AN ANTAGONIST OF SUBSTANCE P
FR2728169A1 (en) 1994-12-19 1996-06-21 Oreal USE OF A SUBSTANCE P ANTAGONIST FOR THE TREATMENT OF PRURITUS AND EYE OR PALPEBRAL DYSESTHESIA
FR2728165A1 (en) 1994-12-19 1996-06-21 Oreal USE OF AN ANTAGONIST OF SUBSTANCE P FOR THE TREATMENT OF SKIN REDNESS OF NEUROGENIC ORIGIN
TW458774B (en) 1995-10-20 2001-10-11 Pfizer Antiemetic pharmaceutical compositions
FR2741262B1 (en) 1995-11-20 1999-03-05 Oreal USE OF A TNF-ALPHA ANTAGONIST FOR THE TREATMENT OF CUTANEOUS REDNESS OF NEUROGENIC ORIGIN
US5750549A (en) * 1996-10-15 1998-05-12 Merck & Co., Inc. Cycloalkyl tachykinin receptor antagonists
US5961987A (en) * 1996-10-31 1999-10-05 University Of Iowa Research Foundation Ocular protein stimulants
EP0942729B1 (en) * 1996-12-02 2004-09-01 MERCK SHARP & DOHME LTD. Use of nk-1 receptor antagonists for treating stress disorders
US5977139A (en) * 1996-12-15 1999-11-02 Hoechst Marion Roussel, Inc. Carboxysubstituted cyclic carboxamide derivatives
US6087348A (en) * 1997-12-01 2000-07-11 Merck Sharp & Dohme Ltd. Use of NK-1 receptor antagonists for treating stress disorders
DE19936789A1 (en) * 1999-08-09 2001-03-01 Vectron Therapeutics Ag New pyrrolidinols and their use in tumor therapy
JP4907818B2 (en) 1999-11-03 2012-04-04 エーエムアール テクノロジー インコーポレイテッド Aryl and heteroaryl substituted tetrahydroisoquinolines and their use to prevent reuptake of norepinephrine, dopamine and serotonin
US7163949B1 (en) 1999-11-03 2007-01-16 Amr Technology, Inc. 4-phenyl substituted tetrahydroisoquinolines and use thereof
CN100430401C (en) 2000-07-11 2008-11-05 Amr科技公司 Novel 4-phenyl substituted tetrahydroisoquinolines and therapeutic use thereof
WO2003057668A1 (en) * 2001-12-28 2003-07-17 Takeda Chemical Industries, Ltd. Nitrogenous cyclic ketone derivative, process for producing the same, and use
TWI283241B (en) * 2002-05-29 2007-07-01 Tanabe Seiyaku Co Novel piperidine compound
EP1756056A1 (en) 2004-06-08 2007-02-28 Pfizer Products Inc. Aza-bicyclo[3.1.0]hex-1-yl derivatives active as nk1 antagonists
RU2388751C2 (en) 2004-07-15 2010-05-10 Амр Текнолоджи, Инк. Aryl- and heteroaryl-substituted tetrahydroisoquinolines and use thereof for inhibiting norepinephrine, dopamine and serotonin reuptake
ES2382814T3 (en) 2005-05-17 2012-06-13 Merck Sharp & Dohme Ltd. Cis-4 - [(4-chlorophenyl) sulfonyl] -4- (2,5-difluorophenyl) cyclohexanopropanoic acid for cancer treatment
EA019115B1 (en) 2005-07-15 2014-01-30 Олбани Молекьюлар Рисерч, Инк. Aryl-and heteroaryl-substituted tetrahydrobenzazepines and use thereof to block reuptake of norepinephrine, dopamine, and serotonin
CN101277960A (en) 2005-09-29 2008-10-01 默克公司 Acylated spiropiperidine derivatives as melanocortin-4 receptor modulators
GB0603041D0 (en) 2006-02-15 2006-03-29 Angeletti P Ist Richerche Bio Therapeutic compounds
GB0606985D0 (en) 2006-04-07 2006-05-17 Merck Sharp & Dohme Therapeutic agents
WO2007125364A1 (en) * 2006-04-26 2007-11-08 Merck Sharp & Dohme Limited Piperidines and related compounds for treatment of alzheimer’s disease
EP2698157B1 (en) 2006-09-22 2015-05-20 Merck Sharp & Dohme Corp. Method of treatment using fatty acid synthesis inhibitors
US20110218176A1 (en) 2006-11-01 2011-09-08 Barbara Brooke Jennings-Spring Compounds, methods, and treatments for abnormal signaling pathways for prenatal and postnatal development
EP2805945B1 (en) 2007-01-10 2019-04-03 MSD Italia S.r.l. Amide substituted indazoles as poly(ADP-ribose)polymerase (PARP) inhibitors
KR20090112722A (en) 2007-01-24 2009-10-28 글락소 그룹 리미티드 3,5-diamino-6- (2,3-dichlorophenyl) -1,2,4-triazine or R (-)-2,4-diamino-5- (2,3-dichlorophenyl)- Pharmaceutical composition comprising 6-fluoromethyl pyrimidine and NX1
WO2008120653A1 (en) 2007-04-02 2008-10-09 Banyu Pharmaceutical Co., Ltd. Indoledione derivative
US8389553B2 (en) 2007-06-27 2013-03-05 Merck Sharp & Dohme Corp. 4-carboxybenzylamino derivatives as histone deacetylase inhibitors
US9156812B2 (en) 2008-06-04 2015-10-13 Bristol-Myers Squibb Company Crystalline form of 6-[(4S)-2-methyl-4-(2-naphthyl)-1,2,3,4-tetrahydroisoquinolin-7-yl]pyridazin-3-amine
AR071997A1 (en) 2008-06-04 2010-07-28 Bristol Myers Squibb Co CRYSTAL FORM OF 6 - ((4S) -2-METHYL-4- (2-NAFTIL) -1,2,3,4-TETRAHYDROISOQUINOLIN-7-IL) PIRIDAZIN-3-AMINA
UA105182C2 (en) 2008-07-03 2014-04-25 Ньюрексон, Інк. Benzoxazines, benzothiazines, and related compounds having nos inhibitory activity
JP5635991B2 (en) 2008-10-30 2014-12-03 メルク・シャープ・アンド・ドーム・コーポレーションMerck Sharp & Dohme Corp. Isonicotinamide orexin receptor antagonist
US8691825B2 (en) 2009-04-01 2014-04-08 Merck Sharp & Dohme Corp. Inhibitors of AKT activity
KR20120034644A (en) 2009-05-12 2012-04-12 알바니 몰레큘라 리써치, 인크. Aryl, heteroaryl, and heterocycle substituted tetrahydroisoquinolines and use thereof
WO2010132487A1 (en) 2009-05-12 2010-11-18 Bristol-Myers Squibb Company CRYSTALLINE FORMS OF (S)-7-([1,2,4]TRIAZOLO[1,5-a]PYRIDIN-6-YL)-4-(3,4-DICHLOROHPHENYL)-1,2,3,4-TETRAHYDROISOQUINOLINE AND USE THEREOF
CA2760837C (en) 2009-05-12 2018-04-03 Albany Molecular Research, Inc. 7-([1,2,4]triazolo[1,5-.alpha.]pyridin-6-yl)-4-(3,4-dichlorophenyl)-1,2,3,4-tetrahydroisoquinoline and use thereof
BR112012008849A2 (en) 2009-10-14 2015-09-22 Schering Corp compound, pharmaceutical composition, and use of a compound
US8999957B2 (en) 2010-06-24 2015-04-07 Merck Sharp & Dohme Corp. Heterocyclic compounds as ERK inhibitors
US8518907B2 (en) 2010-08-02 2013-08-27 Merck Sharp & Dohme Corp. RNA interference mediated inhibition of catenin (cadherin-associated protein), beta 1 (CTNNB1) gene expression using short interfering nucleic acid (siNA)
EP3587574B1 (en) 2010-08-17 2022-03-16 Sirna Therapeutics, Inc. Rna interference mediated inhibition of hepatitis b virus (hbv) gene expression using short interfering nucleic acid (sina)
EP2608669B1 (en) 2010-08-23 2016-06-22 Merck Sharp & Dohme Corp. NOVEL PYRAZOLO[1,5-a]PYRIMIDINE DERIVATIVES AS mTOR INHIBITORS
WO2012030685A2 (en) 2010-09-01 2012-03-08 Schering Corporation Indazole derivatives useful as erk inhibitors
US9242981B2 (en) 2010-09-16 2016-01-26 Merck Sharp & Dohme Corp. Fused pyrazole derivatives as novel ERK inhibitors
ES2663009T3 (en) 2010-10-29 2018-04-10 Sirna Therapeutics, Inc. Inhibition of RNA-mediated gene expression using short interference nucleic acids (ANic)
US9351965B2 (en) 2010-12-21 2016-05-31 Merck Sharp & Dohme Corp. Indazole derivatives useful as ERK inhibitors
EP2699567A1 (en) 2011-04-21 2014-02-26 Merck Sharp & Dohme Corp. Insulin-like growth factor-1 receptor inhibitors
AR088352A1 (en) 2011-10-19 2014-05-28 Merck Sharp & Dohme ANTAGONISTS OF THE RECEIVER OF 2-PIRIDILOXI-4-NITRILE OREXINE
WO2013063214A1 (en) 2011-10-27 2013-05-02 Merck Sharp & Dohme Corp. Novel compounds that are erk inhibitors
US20150299696A1 (en) 2012-05-02 2015-10-22 Sirna Therapeutics, Inc. SHORT INTERFERING NUCLEIC ACID (siNA) COMPOSITIONS
BR112015006990A2 (en) 2012-09-28 2017-07-04 Merck Sharp & Dohme compound, pharmaceutical composition, and use of at least one compound
PL2925888T3 (en) 2012-11-28 2018-03-30 Merck Sharp & Dohme Corp. Compositions and methods for treating cancer
WO2014100065A1 (en) 2012-12-20 2014-06-26 Merck Sharp & Dohme Corp. Substituted imidazopyridines as hdm2 inhibitors
US9540377B2 (en) 2013-01-30 2017-01-10 Merck Sharp & Dohme Corp. 2,6,7,8 substituted purines as HDM2 inhibitors
WO2014142761A1 (en) 2013-03-15 2014-09-18 Nanyang Technological University 3-piperidone compounds and their use as neurokinin-1 (nk1) receptor antagonists
US20160194368A1 (en) 2013-09-03 2016-07-07 Moderna Therapeutics, Inc. Circular polynucleotides
WO2018071283A1 (en) 2016-10-12 2018-04-19 Merck Sharp & Dohme Corp. Kdm5 inhibitors
EP3706742B1 (en) 2017-11-08 2023-03-15 Merck Sharp & Dohme LLC Prmt5 inhibitors
WO2019094312A1 (en) 2017-11-08 2019-05-16 Merck Sharp & Dohme Corp. Prmt5 inhibitors
MX2021001486A (en) 2018-08-07 2021-07-15 Merck Sharp & Dohme Llc Prmt5 inhibitors.
EP3833668B1 (en) 2018-08-07 2025-03-19 Merck Sharp & Dohme LLC Prmt5 inhibitors
US11981701B2 (en) 2018-08-07 2024-05-14 Merck Sharp & Dohme Llc PRMT5 inhibitors
TW202045476A (en) 2019-02-13 2020-12-16 美商默沙東藥廠 5-alkyl pyrrolidine orexin receptor agonists
WO2020167701A1 (en) 2019-02-13 2020-08-20 Merck Sharp & Dohme Corp. Pyrrolidine orexin receptor agonists
US12312332B2 (en) 2019-08-08 2025-05-27 Merck Sharp & Dohme Llc Heteroaryl pyrrolidine and piperidine orexin receptor agonists
US12441730B2 (en) 2019-12-17 2025-10-14 Merck Sharp & Dohme Llc PRMT5 inhibitors
TW202227417A (en) 2020-08-18 2022-07-16 美商默沙東藥廠 Bicycloheptane pyrrolidine orexin receptor agonists

Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE2365391A1 (en) * 1972-04-10 1974-09-26 Teikoku Hormone Mfg Co Ltd 2-SUBSTITUTED ISOXAZOLIDINES AND THE METHOD OF MANUFACTURING THEM
EP0035743A1 (en) * 1980-03-07 1981-09-16 Sagami Chemical Research Center Process for the preparation of dipeptides
WO1990005729A1 (en) * 1988-11-23 1990-05-31 Pfizer Inc. Quinuclidine therapeutic agents
EP0436334A2 (en) * 1990-01-04 1991-07-10 Pfizer Inc. 3-Aminopiperidine derivatives and related nitrogen containing heterocycles

Patent Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE2365391A1 (en) * 1972-04-10 1974-09-26 Teikoku Hormone Mfg Co Ltd 2-SUBSTITUTED ISOXAZOLIDINES AND THE METHOD OF MANUFACTURING THEM
EP0035743A1 (en) * 1980-03-07 1981-09-16 Sagami Chemical Research Center Process for the preparation of dipeptides
WO1990005729A1 (en) * 1988-11-23 1990-05-31 Pfizer Inc. Quinuclidine therapeutic agents
EP0436334A2 (en) * 1990-01-04 1991-07-10 Pfizer Inc. 3-Aminopiperidine derivatives and related nitrogen containing heterocycles

Non-Patent Citations (7)

* Cited by examiner, † Cited by third party
Title
CHEMICAL ABSTRACTS, vol. 102, no. 15, 15 April 1985, Columbus, Ohio, US; abstract no. 131835V, 'azetidines' page 609 ; *
CHEMICAL ABSTRACTS, vol. 102, no. 17, 29 April 1985, Columbus, Ohio, US; abstract no. 148866G, 'benzenepropylamine derivatives' page 569 ; *
CHEMICAL ABSTRACTS, vol. 112, no. 25, 18 June 1990, Columbus, Ohio, US; abstract no. 235066W, 'preparation of azetidinone derivatives as intermediates for beta-lactam synthesis' page 599 ; *
CHEMICAL ABSTRACTS, vol. 95, no. 13, 28 September 1981, Columbus, Ohio, US; abstract no. 115260P, '3-oxo-beta-lactams' page 677 ; *
CHEMICAL ABSTRACTS, vol. 96, no. 1, 5 July 1982, Columbus, Ohio, US; abstract no. 52167M, 'betalactams' page 607 ; *
JOURNAL OF ORGANIC CHEMISTRY vol. 56, no. 18, 1991, pages 5263 - 5277; 'azetidines and bisazetidines' *
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY vol. 105, no. 20, 1983, pages 6339 - 6342; 'effective route to azetidines from azetidin-2-ones using hydroalanes as specific reducing agents' *

Cited By (8)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
GB2268931A (en) * 1992-07-22 1994-01-26 Merck Sharp & Dohme Azabicyclic tachykinin-receptor antagonists
EP0743939B1 (en) * 1994-02-11 2000-05-10 MERCK SHARP & DOHME LTD. Aralkoxy and aralkylthio substituted azacyclic compounds as tachykinin antagonists
US6235291B1 (en) 1994-05-05 2001-05-22 Societe L'oreal S.A. Use of a substance P antagonist in a cosmetic composition, and the composition thus obtained
US6333042B1 (en) 1994-05-05 2001-12-25 Societe L'oreal S.A. Use of a substance P antagonist in a cosmetic composition, and the composition thus obtained
US6203803B1 (en) 1994-12-14 2001-03-20 Societe L'oreal S.A. Use of a substance P antagonist in a cosmetic composition, and the composition thus obtained
FR2766366A1 (en) * 1997-07-24 1999-01-29 Seppic Sa USE OF AT LEAST ONE LIPOAMINOACID AS AN ANTAGONIST OF THE SUBSTANCE P IN A COSMETIC FORMULATION FOR SOOTHING AND / OR PROTECTING ALL SKIN TYPES AND, IN PARTICULAR, SENSITIVE SKIN
WO2025008409A2 (en) 2023-07-03 2025-01-09 Preeti Jha Substituted 2-phenylpiperidine compounds for use in the diagnosis, treatment and/or prevention of cancer
WO2025008409A3 (en) * 2023-07-03 2025-02-13 Preeti Jha Substituted 2-phenylpiperidine compounds for use in the diagnosis, treatment and/or prevention of cancer

Also Published As

Publication number Publication date
ATE136885T1 (en) 1996-05-15
AU2413892A (en) 1993-03-16
IL102833A0 (en) 1993-01-31
DE69210029T2 (en) 1997-01-09
EP0600952B1 (en) 1996-04-17
DE69210029D1 (en) 1996-05-23
EP0600952A1 (en) 1994-06-15
US5459270A (en) 1995-10-17
JPH06510034A (en) 1994-11-10
EP0528495A1 (en) 1993-02-24
AU661711B2 (en) 1995-08-03
CA2112397A1 (en) 1993-03-04

Similar Documents

Publication Publication Date Title
EP0600952B1 (en) Azacyclic compounds, processes for their preparation and pharmaceutical compositions containing them
AU678409B2 (en) 4-arylmethyloxymethyl piperidines as tachykinin antagonists
AU675447B2 (en) Carboxamidomethyl piperidine and analogues
EP0593615B1 (en) Aromatic compounds, compositions containing them and their use in therapy
US5665883A (en) Aralkoxy and aralkylthio substituted azacyclic compounds as tachykinin antagonists
AU2002258414B2 (en) Acylated piperidine derivatives as melanocortin-4 receptor agonists
EP0374801B1 (en) Novel N-sustituted azaheterocyclic carboxylic acids
AU4076593A (en) Azacyclic compounds
NO178187B (en) Analogous Process for Preparation of Therapeutically Active 3-Aminopiperidine Derivatives and Related Nitrogen-Containing Heterocyclic Compounds
KR100586327B1 (en) Method for preparing (R) -α- (2,3-dimethoxyphenyl) -1- [2- (4-fluorophenyl) ethyl] -4-piperidinemethanol
JP2002532480A (en) Morpholinone and morpholine derivatives and uses thereof
US20040210061A1 (en) Novel processes for the preparation of (R)-alpha-(2,3-dimethoxyphenyl)-1-[2-(4-fluorophenyl) ethyl]-4-piperidinemethanol
JPWO2001070689A1 (en) Diphenylalkylamine derivatives useful as opioid delta receptor agonists

Legal Events

Date Code Title Description
AK Designated states

Kind code of ref document: A1

Designated state(s): AT AU BB BG BR CA CH CS DE DK ES FI GB HU JP KP KR LK LU MG MN MW NL NO PL RO RU SD SE US

AL Designated countries for regional patents

Kind code of ref document: A1

Designated state(s): AT BE CH DE DK ES FR GB GR IE IT LU MC NL SE BF BJ CF CG CI CM GA GN ML MR SN TD TG

DFPE Request for preliminary examination filed prior to expiration of 19th month from priority date (pct application filed before 20040101)
WWE Wipo information: entry into national phase

Ref document number: 1992917251

Country of ref document: EP

WWE Wipo information: entry into national phase

Ref document number: 2112397

Country of ref document: CA

WWE Wipo information: entry into national phase

Ref document number: 08196269

Country of ref document: US

WWP Wipo information: published in national office

Ref document number: 1992917251

Country of ref document: EP

REG Reference to national code

Ref country code: DE

Ref legal event code: 8642

WWG Wipo information: grant in national office

Ref document number: 1992917251

Country of ref document: EP